Treatment of patients with multiple sclerosis based on gene expression changes in central nervous system tissues

ABSTRACT

The present invention identifies a number of gene markers whose expression is altered in multiple sclerosis (MS). These markers can be used to diagnose or predict MS in subjects, and can be used in the monitoring of therapies. In addition, these genes identify therapeutic targets, the modification of which may prevent MS development or progression.

[0001] The present application claims benefit of priority U.S. Provisional Serial No. 60/414,219, filed Sep. 27, 2002, the entire contents of which are hereby incorporated by reference.

BACKGROUND OF THE INVENTION

[0002] 1. Field of the Invention

[0003] The present invention relates generally to the fields of molecular biology, genomics, immunology and neurobiology. More particularly, it concerns the identification of specific genes that are dysregulated in patients afflicted with multiple sclerosis (MS), and the use of these genes as targets for MS therapies.

[0004] 2. Description of Related Art

[0005] Multiple sclerosis (MS) continues to be a serious health problem that afflicts hundreds of thousands each year in the US alone, and millions worldwide. One of the difficult aspects of dealing with MS is identifying patients early in the course of the disease. This is difficult not only because of the lack of a definitive biological test for MS, but because the symptoms may overlap with those of numerous other diseases.

[0006] The concordance rate of multiple sclerosis among monozygotic twins is 20-40%, while the risk of a non-twin sibling of an MS patient of developing MS is 2-4%. These facts highly suggest the presence of polygenic susceptibility (nonmendelian inheritance). Although no single gene is associated with all types of MS, several reports have revealed that some genes are associated with MS in certain populations. The well known HLA association with MS has been demonstrated in populations of northern European ancestry. In the Finnish population an association with the myelin basic protein gene has been reported (Tienari et al., 1992). In an European MS patient population, an association with a T cell differentiation-related antigen, CD45, has been demonstrated (Jacobsen et al., 2000).

[0007] Since the disease is polymorphic (i.e., not inherited in a classical mendelian pattern but clearly multiple genes are involved in leading to predisposition), recent genomic approaches have been implemented to elucidate multiple genes simultaneously that may be associated with the disease. A recent publication by Lock et al. (2002) demonstrates how gene expression profiling using DNA microarrays to examine MS brain tissues can help identify multiple single genes that are associated with the disease, and may therefore serve as targets of treatment. By altering the function of the product of some of these genes in the animal model of MS, experimental autoimmune encephalomyelitis (EAE), these authors confirmed that some genes found to be altered by DNA microarray screening indeed had an impact on the severity of the disease.

[0008] Another approach to identify potential single gene associations is to examine polymorphic gene variants or single nucleotide polymorphisms (SNPs) of candidate genes, or screen the entire genome to establish the SNPs that are associated with the disease. Multiple polymorphisms have been associated with MS, as follows: (a) polymorphisms associated with MS disease susceptibility found in the following genes: SCA2 (Chataway et al., 1999), interferon α (Miterski et al., 1999), estrogen receptor (Niino et al., 2000), plasminogen activator inhibitor 1 (Luomala et al., 2000), tumor necrosis factor α (Fernandez-Arquero et al., 1999; Lucotte et al., 2000), monocyte chemotactic protein 3 (Fiten et al., 1999), vitamin D receptor (Fukazawa et al., 1999), CTLA4 (Fukazawa et al., 1999), γ aminobutyric acid (Gade-Andavolu et al., 1998); (b) polymorphisms associated with disease severity found in the following genes: interleukin 6 (Vandenbroeck et al., 2000), IgG Fc receptor (FcγR) (Myhr et al., 1999), glutathione-S-transferase (Mann et al., 2000); (c) polymorphisms associated with age of onset of MS found in the following genes: interleukin 4 (Vandenbroeck et al., 1997) and chemokine receptor CCR5 (Barcellos et al., 2000); and (d) polymorphism associated with remyelination capacity: apolipoprotein E (Carlin et al., 2000). Other gene polymorphisms that have been associated with MS include intercellular adhesion molecule 1 (ICAM-1) (Mycko et al., 1998), the pro-inflammatory gene lymphotoxin (Mycko et al., 1998) and immunoglobulin heavy chain gene polymorphisms (Hashimoto et al., 1993; Walter et al., 1991).

[0009] Despite these individual associations, there has yet to be put forth a cohesive set of genes that provide clearly relevant targets for genetic based therapies.

SUMMARY OF THE INVENTION

[0010] Thus, in accordance with the present invention, there is provided a method for treating or preventing multiple sclerosis (MS) comprising administering to a subject with MS a composition that causes an increase in the level of a gene product selected from the group consisting of those genes indicated by a minus (−) sign in Tables 1-15, except those indicated by asterisk(s). In still yet a further embodiment, there is provided a method for treating or preventing multiple sclerosis (MS) comprising administering to a subject with MS a composition that causes a decrease in the level of a gene product selected from the group consisting of those genes indicated by a plus (+) sign in Tables 1-15, except those indicated by asterisk(s). Further, genes from Table 16, 17, or 18 are lists of genes previously reported to be associated with MS central nervous system tissues by Lock et al. (2002), Chabas et al. (2001), and Whitney et al. (1999), respectively, and are indicated by asterisks in Tables 1-15 as also found by the presented inventors to be dysregulated in MS spinal cords, may be used as targets in combination with one or more of the genes from Tables 1-15.

[0011] The inventors also found, quite strikingly, that the CD18 (probe set X64072, also represented by accession number M15395) subunit of lymphocyte function antigen-1 (LFA-1) and of CR3 and CR4 complement, is highly upregulated in all MS samples (including samples with minimal or no inflammation by histological criteria). CD18 plays a role in immune cell activation, cell-cell contacts and as a mediator of phagocytosis. Bowen et al. (1998) reported a Phase I study using humanized monoclonal antibodies against CD18 protein in MS patients. In addition, Yusuf-Makagiansar et al. (2002) proposed the use of antibodies, peptides and small molecules against CD18 protein to treat autoimmune diseases and inflammation. The present inventors intention, based on striking findings of CD18 mRNA elevation in MS spinal cords, is to target the expression of CD18 mRNA, not protein, in MS central nervous system tissues using technologies such as antisense constructs, RNA interference and other methods described further below.

BRIEF DESCRIPTION OF THE DRAWINGS

[0012] The following drawings form part of the present specification and are included to further demonstrate certain aspects of the present invention. The invention may be better understood by reference to one or more of these drawings in combination with the detailed description of specific embodiments presented herein.

[0013]FIG. 1 Kernel density estimate based on five ratios.

[0014]FIGS. 2A & 2B Kernel density estimate and histogram of ratios with an adjusted bandwidth.

DESCRIPTION OF ILLUSTRATIVE EMBODIMENTS

[0015] In autoimmune diseases, activated T and B cells are hypothesized to clonally expand (i.e., proliferate into multiple daughter cells) and lead to tissue destruction, via infiltration of target tissues with direct cytotoxicity and/or release of harming soluble factors or antibodies. Macrophages are also important mediators of tissue damage. MS is widely considered an autoimmune disease, but there is significant controversy about the key molecules that participate in such process. It also is a heterogeneous disease, and within a single patient, one finds different degrees (and localization in anatomical regions) of demyelination, inflammation and degeneration. The inventors thus examined post-mortem spinal cords via histopathology techniques to determine what type of multiple sclerosis lesions they were working with. Using DNA microarrays, they then determined (by comparing each sample to the average of normal spinal cord samples) the gene expression changes that were unique to each type of MS lesion.

[0016] The results reveal that histopathologically different MS spinal cord lesions also exhibit distinct gene expression changes. Thus, gene lists, as set forth in the Tables below, result from the analysis of: (Table 1) MS spinal cord gray matter from a sample with minimal to no inflammation; (Table 2) MS spinal cord gray matter from a sample with lymphocytic inflammation, demyelination and axonal loss; (Table 3) MS spinal cord gray matter from a sample characterized by inflammation by lymphocytes and macrophages, and demyelination; (4) MS spinal cord gray matter from a sample with axonal loss; (Table 5) MS spinal cord white matter from a sample with minimal to no inflammation; (Table 6) MS spinal cord white matter from a sample with lymphocytic inflammation, demyelination and axonal loss; (Table 7) MS spinal cord white matter from a sample with inflammation by macrophages and demyelination; (Table 8) MS spinal cord white matter from a sample with inflammation by macrophages and lymphocytes and demyelination; and (Table 9) MS spinal cord white matter from a sample with axonal loss. In addition, the inventors provide tables of genes altered in (Table 10) a comparison of the group containing all MS spinal cord gray matter specimens against the group containing all normal gray matter specimens, and (Table 11) a comparison of the group containing all MS spinal cord white matter specimens against the group containing all normal white matter specimens. Also, genes altered commonly across all tables for gray matter (Table 12), white matter (Table 13), and gray & white matter (Table 14) are provided. Table 15 lists genes commonly altered across all comparisons of MS spinal cord white matter characterized by inflammation and demyelination, against normal spinal cord white matter tissues. Table 16, 17 and 18 list genes previously reported to be altered in MS brain tissues by, respectively, Lock et al. (2002) (indicated by one asterisk next to a gene identifier in Tables 1-15), Chabas et al. (2001) (indicated by two asterisks next to a gene identifier in Tables 1-15), and Whitney et al. (1999) (indicated by three asterisks next to a gene identifier in Tables 1-15), and also found by the inventors to be altered (i.e., coregulated and commonly shared) in MS spinal cord tissues. These genes are claimed as targets of treatment only in combination with other genes provided in the inventors' lists (and not in combination with other genes from lists by Lock et al. (2002), Chabas et al. (2001), or Whitney et al. (1999)).

[0017] I. Multiple Sclerosis

[0018] Multiple Sclerosis (MS) is one of the most common diseases of the central nervous system (brain and spinal cord). It is an inflammatory condition associated with demyelination, or loss of the myelin sheath. Myelin, a fatty material that insulates nerves, acts as insulator in allowing nerves to transmit impulses from one point to another. In MS, the loss of myelin is accompanied by a disruption in the ability of the nerves to conduct electrical impulses to and from the brain and this produces the various symptoms of MS, such as impairments in vision, muscle coordination, strength, sensation, speech and swallowing, bladder control, sexuality and cognitive function. The plaques or lesions where myelin is lost appear as hardened, scar-like areas. These scars appear at different times and in different areas of the brain and spinal cord, hence the term “multiple” sclerosis, literally meaning many scars.

[0019] Currently, there is no single laboratory test, symptom, or physical finding that provides a conclusive diagnosis of MS. To complicate matters, symptoms of MS can easily be confused with a wide variety of other diseases such as acute disseminated encephalomyelitis, Lyme disease, HIV-associated myelopathy, HTLV-I-associated myelopathy, neurosyphilis, progressive multifocal leukoencephalopathy, systemic lupus erythematosus, polyarteritis nodosa, Sjögren's syndrome, Behçet's disease, sarcoidosis, paraneoplastic syndromes, subacute combined degeneration of cord, subacute myelo-optic neuropathy, adrenomyeloneuropathy, spinocerebellar syndromes, hereditary spastic paraparesis/primary lateral sclerosis, strokes, tumors, arteriovenous malformations, arachnoid cysts, Arnold-Chiari malformations, and cervical spondylosis. Consequently, the diagnosis of MS must be made by a process that demonstrates findings that are consistent with MS, and also rules out other causes.

[0020] Generally, the diagnosis of MS relies on two criteria. First, there must have been two attacks at least one month apart. An attack, also known as an exacerbation, flare, or relapse, is a sudden appearance of or worsening of an MS symptom or symptoms which lasts at least 24 hours. Second, there must be more than one area of damage to central nervous system myelin sheath. Damage to sheath must have occurred at more than one point in time and not have been caused by any other disease that can cause demyelination or similar neurologic symptoms. MRI (magnetic resonance imaging) currently is the preferred method of imaging the brain to detect the presence of plaques or scarring caused by MS.

[0021] The diagnosis of MS cannot be made, however, solely on the basis of MRI. Other diseases can cause comparable lesions in the brain that resemble those caused by MS. Furthermore, the appearance of brain lesions by MRI can be quite heterogeneous in different patients, even resembling brain or spinal cord tumors in some. In addition, a normal MRI scan does not rule out a diagnosis of MS, as a small number of patients with confirmed MS do not show any lesions in the brain on MRI. These individuals often have spinal cord lesions or lesions which cannot be detected by MRI. As a result, it is critical that a thorough clinical exam also include a patient history and functional testing. This should cover mental, emotional, and language functions, movement and coordination, vision, balance, and the functions of the five senses. Sex, birthplace, family history, and age of the person when symptoms first began are also important considerations. Other tests, including evoked potentials (electrical diagnostic studies that may reveal delays in central nervous system conduction times), cerebrospinal fluid (seeking the presence of clonally-expanded immunoglobulin genes, referred to as oligoclonal bands), and blood (to rule out other causes), may be required in certain cases.

[0022] II. MS-Related Genes

[0023] In the following pages, the applicants set forth gene targets that may be targeted with therapies for MS. Also included are the particular probes utilized to identify these targets.

[0024] In the following tables, a positive value or a plus (+) sign for a log₁₀(ratio)-fold change value, or next to a probe set or gene name, indicates higher expression observed in patients with MS, as compared to healthy individuals. A negative value or a minus (−) sign for a log₁₀(ratio)-fold change value, or next to a probe set or gene name indicates lower expression observed in patients with MS, as compared to healthy individuals.

[0025] The inventors provide herein gene lists of altered mRNA transcripts in individual comparisons of gray or white matter tissue samples derived from MS spinal cord against normal spinal cord tissues (Tables 1-9). As stated, the inventors also provide tables of genes altered in a comparison of the entire group containing all MS spinal cord gray matter specimens against the entire group containing normal gray matter specimens (Table 10), and a comparison of the entire group containing all MS spinal cord white matter specimens against the entire group containing normal white matter specimens (Table 11). Finally, the inventors have identified genes that were dysregulated in each list from Tables 1-9, that had a significance of p<0.05. Then, a set of common genes that appeared in all gray/white lists was searched and means of log₁₀-fold changes, and p values calculated. Only 5 commonly dysregulated genes were identified in the MS gray matter comparison lists (shown as Table 12), while 23 dysregulated genes were commonly found in the MS white matter lists (shown as Table 13). Then, using the same method, another set of common genes across all lists (both gray and white) was also identified (shown as Table 14). Finally, since MS disease activity is characterized by inflammation and demyelination, a list of common genes shared by three individual comparisons of MS spinal cord white matter samples (all characterized by inflammation and demyelination) against normal spinal cord white matter samples was generated (Table 15). Finally, Tables 16, 17 and 18 show MS spinal cord tissue genes from the present invention that are commonly regulated and shared with the list of genes altered in MS tissues by Lock et al. (2002), Chabas et al. (2001), and Whitney et al. (1999). These genes are also shown by asterisk(s) preceding the probe set number in Tables 1-15, as follows: shared with the report by Lock et al. (one asterisk, Table 16), shared with the report by Chabas et al. (two asterisks, Table 17), and shared with the report by Whitney et al. (three asterisks, Table 18). The numbers under “Probe Sets” represent the GenBank accession numbers or, in some instances, an identifier provided by Affymetrix. TABLE 1 Gene targets in MS spinal cord gray matter from a sample with minimal to no histological inflammation. Probe Set Gene description log10 (ratio) fold change M77829 Channel-like integral membrane prot (CHIP28); Also: S73482 2.1973319000 X95406 Cyclin E −2.4820424000 U09937 Urokinase-type plasminogen activator receptor; Also: X51675 −2.4221999000 M25280 Lymph node homing receptor 2.0461048000 *X64072 CD18; Also: M15395 2.0293838000 M21305 Alpha satellite and satellite 3 junction DNA sequence −2.2956496000 M68864 ORF −2.1876265000 M64788 GTPase activating protein (rap1GAP) 1.9611837000 *M87789 Hybridoma H210 anti-hepatitis A IgG V, C, CDR regions 1.9385197000 U78793 Folate receptor alpha (hFR)/U78793 −2.1603560000 D55696 Cysteine protease 1.9194646000 U02031 Sterol regulatory element binding protein-2 1.9049812000 M98045 Folylpolyglutamate synthetase −2.1298107000 X57351 1-8D from interferon-inducible family −2.1186367000 D86971 KIAA0217 1.8382249000 M37457 Na+, K+-ATPase catalytic subunit alpha-III isoform 1.8061800000 M37755 Pregnancy-specific beta-1-glycoprotein PSGGA −2.0861373000 X53414 Peroxisomal L-alanine:glyoxylate aminotransferase −2.0852014000 J04501 Muscle glycogen synthase 1.8014037000 D45906 LIMK-2 −2.0813473000 U60800 Semaphorin (CD100) 1.7899331000 Z84718 DNA on chromosome 22q 11.2-qter contains GSTT1-2 1.7710628000 M13207 Granulocyte-macrophage colony-stimulating factor (CSF1) −2.0635210000 M97252 Kallmann syndrome (KAL) 1.7542944000 U39573 Salivary peroxidase −2.0552349000 J03600 Lipoxygenase −2.0488301000 U56816 Kinase Myt1 (Myt1) −2.0437060000 X17360 HOX 5.1 protein 1.7295697000 Z19002 PLZF kruppel-like zinc finger protein −2.0348289000 U70732 Glutamate pyruvate transaminase (GPT) 1.7155044000 L02648 (clone V6) transcobalamin II (TCN2) −2.0310043000 M16707 Histone H4; clone FO108 −2.0251522000 L14812 Retinoblastoma related protein (p107) −2.0221189000 U73799 Dynactin/U73799 1.6954817000 D28383 ATP synthase B chain 1.6825045000 D50550 LLGL 1.6771760000 M95929 Homeobox protein (PHOX1) 1.6766936000 HG1019-HT1019 Serine Kinase Psk-H1 −2.0052342000 U91327 Chromosome 12p15 BAC clone CIT987SK-99D8 sequence 1.6707096000 M64231 Spermidine synthase −1.9982048000 U79725 A33 antigen precursor −2.0023281000 D16583 L-histidine decarboxylase 1.6622855000 U68723 Checkpoint suppressor 1 1.6419879000 U94747 WD repeat protein HAN11/U94747 1.6329632000 U49089 Neuroendocrine-dlg (NE-dlg) −1.9643186000 U22970 16-Jun (interferon-inducible peptide precursor) −1.9576671000 X86681 Nucleolar protein HNP36 −1.9585042000 HG2147-HT2217 Mucin 3, Intestinal/M55405 −1.9540012000 X14474 Microtubule-associated tau protein 1.5998831000 D55638 B-cell pseudoautosomal boundary-like sequence −1.9438653000 M58597 ELAM-1 ligand fucosyltransferase (ELFT) −1.9472499000 U37519 Aldehyde dehydrogenase (ALDH8) −1.9341827000 HG651-HT5209 Adducin, Alpha Subunit; Also: Z68280_2, HG651-HT4201 1.5820634000 M13928 X64467_rna1 and others 1.5757650000 M63573 Secreted cyclophilin-like protein (SCYLP) 1.5763414000 U48861 Beta 4 nicotinic acetylcholine receptor subunit 1.5711263000 M12125 Fibroblast muscle-type tropomyosin −1.9227255000 Z80780 H2B/h/Z80780 1.5641730000 D84454 UDP-galactose translocator 1.5618030000 X96783 Syt V 1.5599066000 X13810 OTF-2 lymphoid-specific transcription factor; Also: M36542 −1.9130850000 X52611 Transcription factor AP-2; Also: HG2465-HT4871, M36711 −1.9158613000 AF000545 Putative purinergic receptor P2Y10 −1.9043097000 L35240 Enigma 1.5440680000 X81420 hHKb1 protein 1.5432976000 D28532 Renal Na+-dependent phosphate cotransporter −1.8974209000 X63692 DNA (cytosin-5)-methyltransferase 1.5308398000 J05448 RNA polymerase subunit hRPB 33 1.5199493000 U31628 Interleukin-15 receptor alpha chain precursor (IL15RA) 1.5214458000 D43968 AML1b protein −1.8803133000 M13232 Factor VII serine protease precursor; Also: J02933 −1.8815986000 U57450 EPC-1 −1.8814560000 U29091 Selenium-binding protein (hSBP)/U29091 1.5158738000 Y07755 S100A2 −1.8752784000 X16667 HOX2G from the Hox2 locus −1.8693784000 HG3033-HT3194 Spliceosomal protein Sap 62 1.5048795000 X52213 ltk; Also: D16105 1.5037907000 X01038 Fetal apolipoprot AI precursor; Also: X07496 −1.8629658000 U64197 Chemokine exodus −1.8589881000 HG2709-HT2805 Serine/Threonine Kinase 1.4913617000 D29642 KIAA0053 1.4694538000 L11708 17 beta hydroxysteroid dehydrogenase type 2 −1.8364032000 D38502 PMS4 (yeast PMS1 homolog) 1.4631461000 *M85220 Heavy chain disease IgA chain CH3 region 1.4556061000 M60299 Alpha-1 collagen type II s 1 2 and 3 −1.8246952000 M73481 Gastrin releasing peptide receptor (GRPR) −1.8188030000 D26350 Type 2 inositol 1 4 5-trisphosphate receptor 1.4471580000 X90840 Axonal transporter of synaptic vesicles −1.8153287000 D59253 NCBP interacting protein 1 1.4369573000 X17651 Myf-4 myogenic determination factor 1.4310639000 M95178 Non-muscle alpha-actinin 1.4240645000 L32866 Effector cell protease receptor-1 (EPR-1) −1.8044802000 X87871 Hepatocyte nuclear factor 4b; Also: X87870, Z49825 −1.8050759000 HG2510-HT2606 Ras-Specific Guanine Nucleotide-Releasing Factor 1.4210614000 M60298 Erythrocyte membrane protein band 42 (EPB42) 1.4132998000 AF003743 Delayed rectifier potassium channel (KVLQT1-Iso5) −1.7940211000 U07139 Voltage-gated calcium channel beta subunit 1.4040622000 U33429 K+ channel beta 2 subunit 1.4052248000 L00205 K6b epidermal keratin type II −1.7875490000 U04847 Ini1 −1.7896688000 U58090 Hs-cul-4A 1.3944517000 U07919 Aldehyde dehydrogenase 6 −1.7871717000 X59798 PRAD1 cyclin 1.3906515000 U78190 GTP cyclohydrolase I feedback regulatory protein −1.7774268000 D79998 KIAA0176 −1.7700231000 D82344 NBPhox −1.7704838000 HG919-HT919 Dna Polymerase Epsilon Catalytic Subunit −1.7714956000 U03911 Mutator (hMSH2) 1.3594190000 U24169 JTV-1 (JTV-1) 1.3614459000 U71364 Serine protase inhibitor (P19) 1.3598355000 S79781 WT1/S79781 −1.7641855000 M31606 Phosphorylase kinase (PSK-C3) 1.3473300000 M95740 Alpha-L-iduronidase 1.3443923000 M27492 Interleukin 1 receptor −1.7547305000 AD000092 RAD23A homolog 1.3262746000 Y08613 Nup88/Y08613 −1.7490596000 M59820 Granulocyte colony-stimulating factor receptor (CSF3R) 1.3031961000 L04751 Cytochrome p-450 4A (CYP4A) −1.7450748000 U28281 Secretin receptor −1.7464396000 X63380 RSRFR2 1.3004888000 U13737 Cysteine protease CPP32 isom alpha −1.7422340000 M80647 Thromboxane synthase 1.2811352000 X54871 Ras-related protein Rab5b 1.2810334000 X14445 Int-2 protooncogene −1.7359979000 HG1996-HT2044 Guanine Nucleotide-Binding protein Rap2 1.2741578000 M95809 Basic TRANSCRIPTION FACTOR 62 kD subunit (BTF2) 1.2684286000 D43772 GRB-7 SH2 domain −1.7320317000 M12886 T-cell receptor active beta-chain −1.7301764000 M18700 D00306, M16630, M18692 −1.7273379000 U49974 Mariner2 transposable element, complete consensus/U49974 −1.7266253000 HG3748-HT4018 Basic Transcription Factor 44 Kda Subunit 1.2504200000 AF015950 Telomerase reverse transcriptase 1.2348010000 HG172-HT3924 Spermidine/Spermine N1-Acetyltransferase −1.7147488000 HG4749-HT5197 Carnitine Calcium-Binding protein Mitochondrial −1.7155856000 M55905 Mitochondrial NAD(P)+ dependent malic enzyme 1.2188888000 U82987 Bcl-2 binding component 3 (bbc3) 1.2105620000 M21984 (clone PWHTnT16) skeletal muscle Troponin T −1.7104347000 U27333 Alpha (1,3) fucosyltransferase (FUT6), major transcript I −1.7091639000 X52228 Secreted epithelial tumour mucin antigen −1.7084421000 U11313 Sterol carrier protein-X/sterol carrier protein-2 (SCP-X/SCP-2) 1.2041200000 Y08766 Splicing factor, SF1-Bo isoform; Also: L49380 1.2043797000 Z38133 Myosin; Also: M36769 1.2066376000 X06389 Synaptophysin (p38) 1.1958997000 ***J05037 Serine dehydratase 1.1836070000 U66619 SWI/SNF complex 60 KDa subunit (BAF60c) 1.1869136000 AB000462 SH3 binding RES4-23A −1.6994041000 M34344 Platelet glycoprotein IIb (GPIIb) −1.6981938000 U03399 T-complex protein 10A (TCP10A) −1.6989700000 X52599 Beta nerve growth factor −1.6989700000 M14159 T-cell receptor beta-chain J2.1 −1.6935071000 HG880-HT880 MUC6 −1.6893089000 L27080 Melanocortin 5 receptor (MC5R) −1.6898081000 X53795 R2 inducible membrane protein −1.6877853000 J05459 Glutathione transferase M3 (GSTM3) 1.1278244000 M14091 Thyroxine-binding globulin −1.6859655000 U01157 Glucagon-like peptide-1 receptor with CA dinucleotide repeat 1.1080076000 M74542 Aldehyde dehydrogenase type III (ALDHIII) −1.6798819000 D28423 Pre-splicing factor SRp20 1.1074088000 X97748 PTX3/X97748; Also: M31166 1.0958364000 M55621 N-acetylglucosaminyltransferase I (GlcNAc-TI) −1.6770363000 Y07829 RING protein −1.6729056000 Y09561 P2X7 receptor 1.0883800000 S83325 Aspartyl(asparaginyl)beta-hydroxylase; Also: U03109 1.0849797000 D50920 KIAA0130 −1.6678030000 Y10262 EYA3/Y10262; Also: U81602 −1.6676864000 U80457 TRANSCRIPTION FACTOR SIM2 short form 1.0646428000 L41351 Prostasin −1.6632296000 J03068 DNF1552 (lung) 1.0594372000 U62433 Nicotinic acetylcholine receptor alpha4 subunit precursor 1.0592429000 L76528 Presenilin 1 (PS1; S182); Also: L76517 1.0524293000 L38933 Putative with an open reading frame −1.6565773000 S82472 Polymerase beta/S82472 −1.6539357000 M14949 R-ras 1.0389477000 U46746 Dystrobrevin-epsilon; Also: U46744 1.0359475000 X78992 ERF-2 1.0341524000 X76105 DAP-1 1.0298785000 L03840 Fibroblast growth factor receptor 4 (FGFR4); Also: X57205 −1.6517624000 M25077 SS-A/Ro ribonucleoprot autoantigen 60 kd subunit 1.0221579000 X99479 NK receptor, clone 12.11C-Also Similar To: X93596, L76672 −1.6450537000 D13168 Endothelin-B receptor 1.0139885000 HG511-HT511 Ras Inhibitor Inf 1.0134230000 L13698 Growth-arrest-specific protein (gas) 1.0174481000 *U21090 DNA polymerase delta small subunit 1.0132654000 U36448 Ca2+-dependent activator protein secretion 1.0153598000 U82979 Ig-like transcript-3 −1.6332159000 L07592 Peroxisome proliferator activated receptor −1.6308091000 U15932 Dual-specificity protein phosphatase −1.6301735000 U32674 Orphan receptor GPR9 (GPR9); Also: X95876 −1.6318241000 X68090 Fc-gamma-RIIA IgG Fc receptor class IIA/X68090 −1.6294096000 D31764 KIAA0064 0.9738912400 M27543 Guanine nucleotide-binding protein (Gi) alpha subunit 0.9751461800 Z11695 40 kDa protein kinase related to rat ERK2 0.9731278500 D31886 KIAA0066 0.9686520200 HG3985-HT4255 Cpg-Enriched Dna Clone E04 −1.6245399000 D10495 Protein kinase C delta-type 0.9660821500 AB000896 Cadherin FIB2 −1.6193542000 U32581 Lambda/iota-prot kinase C-interacting protein −1.6184404000 U63090 Gal beta-13 GalNAc alpha-23 sialyltransferase (ST3Gal II) −1.6209873000 *D10704 Choline kinase 0.9532953000 D90359 CCG1 0.9501715500 D29675 iNOS −1.6131809000 M63904 G-alpha 16 protein −1.6134650000 D80009 KIAA0187 0.9330532100 Y10260 EYA1 −1.6079909000 Z80345 SCAD; Also: M26393 −1.6091941000 U49188 Placenta (Diff33) 0.9315474000 U23430 Cholecystokinin type A receptor (CCK-A); Also: L19315 0.9255532700 M15465 Pyruvate kinase type L; Also: D13243 −1.6032797000 U17077 BENE −1.6035503000 U41344 Prolargin (PRELP) −1.6028735000 Y08836 HRX-like protein/Y08836 −1.6028735000 L21993 Adenylyl cyclase 0.9201585600 L37127 (clone mf18) RNA polymerase II 0.9208968900 U89916 Putative OSP like protein 0.9140545300 U55054 K-Cl cotransporter (hKCC1) 0.9122979900 L38969 Thrombospondin 3 (THBS3) −1.6019243000 HG3517-HT3711 Alpha-1-Antitrypsin −1.5969543000 U08021 Nicotinamide N-methyltransferase (NNMT) −1.5934245000 U82613 DNA-binding protein ABP/ZF −1.5942544000 X66141 Cardiac ventricular myosin light chain-2 −1.5938900000 X78687 G9 encoding sialidase −1.5934139000 M81182 Peroxisomal 70 kD membrane protein; Also: X83467_rna1 0.8950389800 U09646 Carnitine palmitoyltransferase II precursor (CPT1) 0.8888069700 *U64573 Connexin43 gap junction protein (connexin43)/U64573 0.8848286700 U18237 ATP-binding cassette protein 06B09 clone −1.5917600000 X99720 TPRC 0.8798514200 Z46632 HSPDE4C1 3,5-cyclic AMP phosphodiesterase 0.8815503100 S81294 DCC = deleted in colorectal cancer/S81294 −1.5848963000 X77307 5-HT2B serotonin receptor −1.5841898000 X66362 PCTAIRE-3 serine/threonine protein kinase 0.8690051700 D42053 KIAA0091 0.8599566400 U35139 NECDIN related protein 0.8591271000 U93049 SLP-76 associated protein 0.8613913500 D43947 KIAA0100 0.8530723400 M13903 Involucrin 0.8571154000 M29277 Isolate JuSo MUC18 glycoprot (3 variant); Also: M28882 0.8570771000 D79989 KIAA0167 −1.5764853000 U78876 MEK kinase 3 −1.5733068000 Z83805 Axonemal dynein heavy chain (ID hdhc8)/Z83805 −1.5731618000 U22028 Cytochrome P450 (CYP2A13) 0.8496834500 D87433 KIAA0246 −1.5683484000 U40002 Hormone-sensitive lipase testicular isoform; Also: L11706 −1.5721452000

[0026] TABLE 2 Gene targets in MS spinal cord gray matter from a sample with lymphocytic inflammation, demyelination and axonal loss. Probe set Gene description log10 (ratio) fold change *M87789 Anti-hepatitis A IgG V, C, CDR regions; Also: J00221_2 3.1221503000 Y00067 Neurofilament subunit M (NF-M) −3.0995382000 D13643 KIAA0018 −3.0496210000 *M63438 Ig rearranged gamma chain, V-J-C region; Also: X96754 2.6660416000 L10678 Profilin II −2.6086865000 *U62317 Hypothetical protein 384D8_7 2.2480959000 M22538 Mitochondrial NADH-ubiquinone reductase 24 Kd subunit −2.5507938000 X99657 Protein containing SH3 domain SH3GL2 2.2324879000 X98225 Gastrin-binding protein/X98225 2.2077690000 L07597 Ribosomal protein S6 kinase 2 (RPS6KA2) 2.2060088000 D13705 Fatty acids omega-hydroxylase (cytochrome P-450HKV) −2.4579765000 L14565 Peripherin (PRPH)s 1-9 −2.4614422000 U57341 Neurofilament triplet L protein/U57341 −2.4386017000 U60644 HU-K4 −2.4171186000 Y00757 Polypeptide 7B2 −2.3941670000 D50550 LLGL 2.1022931000 U92457 Metabotropic glutamate receptor 4; Also: X80818 2.1004650000 D63484 KIAA0150 2.0939467000 HG3033-HT3194 Spliceosomal protein Sap 62 2.0822352000 M27749 Ig-related 14.1 protein 2.0722499000 M22632 Mitochondrial aspartate aminotransferase −2.3186893000 X87870 Hepatocyte nuclear factor 4a 2.0546131000 U18244 Excitatory amino acid transporter 4 2.0463000000 *X00734 Beta-tubulin (5-beta) with ten Alu family members −2.2901738000 M22976 Cytochrome b5 −2.2794103000 M57609 DNA-binding protein (GLI3) −2.2654959000 D50663 TCTEL1 −2.2489536000 J05073 Phosphoglycerate mutase (PGAM-M) 1.9672499000 U82987 Bcl-2 binding component 3 (bbc3) 1.9497120000 L35240 Enigma 1.9412629000 S83390 T3 receptor-associating cofactor-1; Also: U37146 1.9278533000 L07738 DHP-sensitive calcium channel gamma subunit (CACNLG) 1.9250541000 D43767 Chemokine −2.2221635000 L40397 (clone S31i125) −2.2061848000 M36542 Lymphoid-specific transcription factor; Also: X13810, X13809 −2.2043574000 U11877 Interleukin-8 receptor type B (IL8RB)/U11877 1.8893017000 J00123 Enkephalin −2.1938895000 X92896 ITBA2 protein −2.1926490000 X15331 Phosphoribosylpyrophosphate synthetase subunit one −2.1855067000 Z21488 Contactin −2.1837679000 U49973 Tigger 1 transposable element 1.8618330000 D16583 L-histidine decarboxylase 1.8518696000 U52969 PEP19 (PCP4) −2.1730770000 **X05299 (˜95%) major centromere autoantigen CENP-B 1.8387444000 X01630 Argininosuccinate synthetase −2.1602058000 D50402 NRAMP1 1.8214780000 J00220 IGHA1 from Ig germline H-chain G-E-A region A: gamma-3 5 1.8210038000 U16031 TRANSCRIPTION FACTOR IL-4 Stat 1.8178958000 X67325 p27 −2.1546522000 M29927 Ornithine aminotransferase −2.1375915000 M87860 S-lac lectin L-14-II (LGALS2) 1.7914660000 M58509 FDXR (adrenodoxin reductase); Also: HG2836-HT2962 1.7833611000 L47345 Elongin A −2.1360464000 M13755 Interferon-induced 17-kDa/15-kDa protein −2.1340391000 HG3928-HT4198 SFTPA2D 1.7625109000 HG2348-HT2444 Peptide Yy; Also: D13897 1.7609311000 L34587 RNA polymerase II elongation factor SIII p15 subunit −2.1126469000 X05608 Neurofilament subunit NF-L −2.1160768000 M95178 Non-muscle alpha-actinin 1.7450748000 D38128 IP prostacyclin receptor 1.7411516000 HG2604-HT2700 Pan-2 1.7415455000 U42408 Ladinin (LAD) 1.7395723000 Z33905 43 kD acetylcholine receptor-associated protein (Rapsyn) 1.7335985000 L41143 Expressed pseudo TCTA at t(1;3) translocation site −2.1054392000 HG4128-HT4398 Anion Exchanger 3 Cardiac Isom 1.7299743000 X64037 RNA polymerase II associated protein RAP74 −2.0997238000 X52638 6-phosphofructo-2-kinase/fructose-26-bisphosphatase −2.0953001000 U72671 Telencephalin precursor 1.7172543000 D85758 DROER homolog −2.0905666000 *L26339 Autoantigen 1.7041505000 U50360 Calcium, calmodulin-dependent protein kinase II gamma −2.0863598000 X53414 Peroxisomal L-alanine: glyoxylate aminotransferase −2.0852014000 U89336 Notch 4 1.6941903000 U79255 X11 protein −2.0789097000 X99142 Hair keratin hHb6 −2.0812573000 D14663 KIAA0107 −2.0728011000 X99897 P/Q-type calcium channel alpha1 subunit; Also: U79663 1.6798819000 J00124 50 kDa type I epidermal keratin −2.0680931000 X04706 Homeobox (clone HHO.c13); Also: X17360 1.6702459000 M13207 Granulocyte-macrophage colony-stimulating factor (CSF1) −2.0635210000 X02761 Fibronectin (FN precursor); Also: HG3044-HT2527 −2.0637086000 U61734 Protein trafficking protein (S31iii125); Also: L40397 −2.0620176000 D50532 Macrophage lectin 2 1.6536841000 L09708 Complement component 2 (C2) allele b 1.6573649000 M74509 HG4045-HT4315 and others −2.0537025000 S72487 Orf1 to PD-ECGF/TPorf2 to PD-ECGF/TP −2.0528382000 X17094 Furin 1.6503075000 *D13988 Rab GDI −2.0496540000 X59842 PBX2; Also: U89336_2, D28769_1, X80700 −2.0479877000 X02958 Interferon alpha IFN-alpha 6 1.6349808000 U35340 Beta B1-crystallin 1.6263404000 L02648 (clone V6) transcobalamin II (TCN2) −2.0310043000 U23803 Heterogeneous ribonucleoprotein A0 −2.0311711000 U91316 Acyl-CoA thioester hydrolase −2.0287237000 M16707 Histone H4; clone FO108 −2.0251522000 M86826 IGF binding protein complex acid-labile subunit a 1.6117233000 X81637 Clathrin light chain b 1.6111921000 U25801 Tax1 binding protein 1.6031444000 M96738 Somatostatin receptor subtype 3 (SSTR3); Also: Z86000 1.5993371000 D49817 Fructose 6-phosphate 2-kinase/fructose 2 6-bisphosphatase −2.0132587000 U73499 Hepatic nuclear factor 1-alpha (TCF-1-alpha)/U73499 1.5929617000 HG2709-HT2805 Serine/Threonine Kinase 1.5910646000 HG4115-HT4385 Olfactory Receptor Or17-210 1.5899496000 S77893 GPSAT = glycophorin SAT; Also: L31860 1.5831988000 D50913 KIAA0123 −2.0061450000 M33882 p78 protein −2.0057702000 X77748 Metabotropic glutamate receptor type 3 −2.0060915000 HG3991-HT4261 Cpg-Enriched Dna, Clone E18 1.5809250000 *U62317 Hypothetical protein 384D8_7 1.5818566000 *J03263 Lysosome-associated membrane glycoprotein (lamp A) −2.0018959000 M81780 SMPD1 1.5735256000 X70070 Neurotensin receptor 1.5770137000 M64925 Palmitoylated erythrocyte membrane protein (MPP1) −1.9929399000 X07315 PP15 (placental protein 15) −1.9968399000 U82279 Ig-like transcript 2 1.5717088000 K03021 Tissue plasminogen activator (PLAT) −1.9892829000 X06956 HALPHA44 alpha-tubulin −1.9917528000 S69370 PAX3B = transcription factor; Also: S69369 1.5611014000 S52969 Alpha-1.3 fucosyltransferase/FucT-III and Fuct-VI −1.9849209000 U32645 Myeloid elf-1 like factor (MEF) 1.5563025000 HG2259-HT2348 Tubulin, Alpha 1; Also: X06956 −1.9746844000 M77810 TRANSCRIPTION FACTOR GATA-2 1.5440680000 U01828 Microtubule-associated protein 2 (MAP2) 1.5378191000 *X64072 CD18; Also: M15395 1.5346606000 X77567 InsP3 5-phosphatase; Also: Z31695 1.5360159000 M21574 Platelet-derived growth factor receptor alpha (PDGFRA) −1.9621325000 U22970 16-Jun (interferon-inducible peptide precursor); Also: U22970 −1.9576671000 U60521 Protease proMch6 (Mch6) −1.9583249000 D38163 a1(XIX) collagen chain; Also: U09279 1.5232039000 D86549 p97 homologous protein −1.9537597000 L36983 Dynamin (DNM) −1.9527319000 S67247 Smooth muscle myosin heavy chain isoform Smemb 1.5204835000 U73799 Dynactin/U73799 1.5198280000 X98258 M-phase phosphoprotein mpp9 1.5211381000 U18671 Stat2 −1.9471273000 U24183 Phosphofructokinase (PFKM); Also: HG1849-HT1878 −1.9432471000 L41939 (clone FBK III 11c) protein-tyrosine kinase (DRT) 1.5047354000 L08069 Heat shock protein E coli DnaJ homolog −1.9388323000 HG4458-HT4727 Ig Heavy Chain Vdjc Regions 1.4976206000 U46767 Monocyte chemoattractant protein-4 precursor (MCP-4) 1.5006024000 U17886 Succinate dehydrogenase iron-protein subunit (sdhB) −1.9363881000 S71018 Cyclophilin C 1.4892552000 D14874 Adrenomedullin −1.9296743000 M62843 Antigen of paraneoplastic sensory neuronopathy patients −1.9305033000 U28488 Putative G protein-coupled receptor (AZ3B); Also: U62027 1.4864470000 X82324 Brain 4 1.4828736000 X52008 Strychnine binding subunit of inhibitory glycine receptor −1.9199275000 *M35999 Platelet glycoprotein IIIa (GPIIIa) 1.4727564000 U08316 Insulin-stimulated protein kinase 1 (ISPK-1) −1.9153998000 X13810 OTF-2 lymphoid-specific transcription factor; Also: M36542 −1.9130850000 M89470 Paired-box protein (PAX2); Also: L25597 −1.9122221000 X03072 Int-1 mammary oncogene −1.9080827000 X66363 PCTAIRE-1 serine/threonine protein kinase −1.9106244000 L14848 MHC class I-related protein; Also: X91625, U65416, X92841 1.4664804000 X97748 PTX3/X97748; Also: M31166 1.4629523000 M21056 Pancreatic phospholipase A-2 (PLA-2) 1.4616772000 M92934 Connective tissue growth factor −1.9045194000 U07620 MAP kinase −1.9057284000 U41668 Deoxyguanosine kinase −1.9062003000 U95006 D9 splice variant A −1.9062677000 M60891 Uroporphyrinogen decarboxylase (URO-D)/M60891 1.4528033000 M86406 Skeletal muscle alpha 2 actinin −1.8953535000 *Y12711 Putative progesterone binding protein −1.8947313000 X15675 pTR7 repetitive sequence/X15675 1.4440448000 Z46788 Cylicin II 1.4471580000 M99438 Transducin-like enhancer protein (TLE3) 1.4392274000 L78833 Ifp35 from Rho7 vatl and BRCA1 −1.8836614000 M94077 Loricrin 1.4364518000 U62433 Nicotinic acetylcholine receptor alpha4 subunit precursor 1.4370998000 K03183 Chorionic gonadotropin beta subunit −1.8803276000 M65085 Follicle stimulating hormone receptor 1.4251925000 X80026 B-cam −1.8752784000 M60459 Erythropoietin receptor 1.4224257000 M64595 Small G protein (Gx) 1.4207806000 U19247 Interferon-gamma receptor alpha chain −1.8687913000 X78992 ERF-2 1.4167905000 L41147 5-HT6 serotonin receptor −1.8638257000 X77794 Cyclin G1 −1.8655481000 U64197 Chemokine exodus −1.8589881000 U81607 Gravin −1.8604129000 *L25270 XE169 1.4063065000 U72507 40871 sequence 1.4070380000 L16991 Thymidylate kinase (CDC8) −1.8551404000 L31573 Sulfite oxidase 1.3947839000 L44140 DNL1L from chromosome X region; Also: X90392 1.3935752000 M63573 Secreted cyclophilin-like protein (SCYLP) 1.3953264000 X51804 PMI a putative receptor protein −1.8500333000 X87176 17-beta-hydroxysteroid dehydrogenase −1.8495730000 U56833 VHL binding protein-1 (VBP-1) −1.8445548000 U53174 Cell cycle checkpoint control protein 1.3829171000 D10925 HM145 1.3812916000 M11321 Group-specific component vitamin D-binding protein 1.3820170000 X90999 Glyoxalase II −1.8350561000 HG1139-HT4910 Fk506-Binding protein 1.3765770000 HG4683-HT5108 Tumor Necrosis Factor Receptor 2 Associated protein Trap3 1.3756148000 M17252 Cytochrome P450c21 1.3773315000 X15954 MBP1; Also: X15422 1.3747483000 U76456 Tissue inhibitor of metalloproteinase 4 1.3694342000 L38487 Estrogen receptor-related protein (hERRa1) −1.8276358000 AF000234 P2x purinoceptor 1.3626709000 HG4051-HT4321 Choline Acetyltransferase 1.3626709000 M27878 DNA binding protein (HPF2) 1.3645510000 U65011 Preferentially expressed antigen of melanoma (PRAME) 1.3652493000 X52896 Dermal fibroblast elastin; Also: HG2994-HT4851 1.3636120000 Z35278 PEBP2aC1 acute myeloid leukaemia 1.3626709000 X89067 Trpc2 transcript (possible pseudo) 1.3586961000 D78275 Proteasome subunit p42 −1.8189678000 L24804 (p23) −1.8218409000 M24594 Interferon-inducible 56 Kd protein −1.8170693000 X90840 Axonal transporter of synaptic vesicles −1.8153287000 HG4557-HT4962 Small Nuclear Ribonucleoprotein U1, 1snrp 1.3434086000 S76067 CNG2 = cyclic nucleotide-gated cation channel/S76067 1.3456620000 D85433 MURR1 −1.8097280000 X12458 P3 1.3414345000 D28383 ATP synthase B chain 1.3369167000 Z84721 DNA from 16p13.3 Contains alpha and zeta globin −1.8031156000 U80017 Survival motor neuron protein 1.3281136000 D42087 KIAA0118 −1.8007171000 J05582 Pancreatic mucin; Also: J05581 −1.8004593000 L00634 Farnesyl-protein transferase alpha-subunit; Also: L10413 −1.7992544000 S80335 Integrin beta 7 subunit 1.3252515000 U67849 Beta-galactoside alpha26-sialyltransferase (SIAT1)/U67849 1.3200240000 HG2815-HT2931 Myosin, Light Chain/U02629; Also: HG2815-HT1357 −1.7970077000 X80343 p35 regulatory subunit of cdk5 kinase 1.3159703000 L43579 (clone 110298)/L43579; Also: L43575 −1.7886985000 M21005 Migration inhibitory factor-related protein 8 (MRP8) −1.7900211000 S74683 ADP-ribosyltransferase −1.7919537000 U07000 BCR (unknown) from breakpoint cluster region (BCR) −1.7916029000 U10117 Endothelial-monocyte activating polypeptide II −1.7917783000 X59417 PROS-27 −1.7922165000 *HG2730-HT2828 Fibrinogen, A Alpha Polypeptide; Also: M58569 1.3053514000 X07203 CD20 receptor (S7) 1.3053088000 D86956 KIAA0201 −1.7865740000 U07151 GTP binding protein (ARL3) −1.7839036000 U73167 H_LUCA146 −1.7841714000 M76180 Aromatic amino acid decarboxylase (ddc) 1.3010300000 Z69923 DNA sequence from Huntington's Disease Region 1.3015718000 D80009 KIAA0187 1.2953744000 M34041 Alpha-2-adrenergic receptor (alpha-2 c2) −1.7816656000 M96956 (clone CR-3) teratocarcinoma-derived growth factor 3 TDGF3 1.2922561000 M59820 Granulocyte colony-stimulating factor receptor (CSF3R) 1.2833012000 HG4258-HT4528 Kinase Inhibitor P27kip1 Cyclin-Dependent −1.7678976000 X57129 H12 histone H1 1.2764618000 *HG1595-HT4788 Heterogeneous Nuclear Ribonucleoprotein I; Also: HG1595-HT4789, 1.2717876000 X66975 M32334 Intercellular adhesion molecule 2 (ICAM-2) −1.7634280000 M98343 Amplaxin (EMS1) −1.7631471000 X69950 DNA sequence for Wilms tumor; Also: M60614 −1.7625848000 AC002450 BAC clone GS244B22/7q21-q22/AC002450 1.2669762000 Z46632 HSPDE4C1 3,5-cyclic AMP phosphodiesterase 1.2671717000

[0027] TABLE 3 Gene targets in MS spinal cord gray matter from a sample characterized by inflammation by lymphocytes and macrophages, and demyelination. Probe set Gene description log10 (ratio) fold change X05608 Neurofilament subunit NF-L −2.9853086000 *M87789 Anti-hepatitis A IgG V, C, CDR regions; Also: J00221_2 3.4707705000 *M63438 Ig rearranged gamma chain V-J-C region; Also: X96754 3.4656016000 L76200 Guanylate kinase (GUK1) −2.5051160000 M34516 Omega light chain protein 14.1 (Ig lambda chain related) 2.5219506000 S68616 Na+/H+ exchanger NHE-1 isom −2.4902746000 L11672 Kruppel related zinc finger protein (HTF10) −2.4847446000 L44140 DNL1L from chromosome X region; Also: X90392 2.2062455000 U57341 Neurofilament triplet L protein/U57341 −2.4386017000 *X13334 CD14 myeloid cell-specific leucine-rich glycoprotein 2.1191968000 M62505 C5a anaphylatoxin receptor 2.0890128000 L28821 Alpha mannosidase II isozyme −2.3860975000 D50402 NRAMP1 2.0422244000 *X64072 CD18; Also: M15395 2.0330818000 M27826 Endogenous retroviral protease −2.3628828000 Z22548 Thiol-specific antioxidant protein −2.3496417000 HG3991-HT4261 Cpg-Enriched Dna, Clone E18 2.0112320000 U28488 Putative G protein-coupled receptor (AZ3B); Also: U62027 1.9889735000 M80397 DNA polymerase delta catalytic subunit; Also: M81735 −2.3239221000 U09210 Vesicular acetylcholine transporter −2.3253617000 J04469 Mitochondrial creatine kinase (CKMT) −2.3121244000 U77643 K12 protein precursor 1.9392946000 U43916 Tumor-associated membrane protein homolog (TMP) 1.9347509000 M27161 MHC class I CD8 alpha-chain (Leu-2/T8) −2.2965281000 *X00734 Beta-tubulin (5-beta) with ten Alu family members −2.2901738000 D00654 Enteric smooth muscle gamma-actin 1.9127421000 HG3286-HT3463 Crystallin Alpha A −2.2734643000 L13266 N-methyl-d-aspartate receptor (NR1-1) −2.2750809000 D49357 S-adenosylmethionine synthetase 1.8856319000 X84213 BAK BCI-2 homolog; Also: U16811, U23765 1.8714562000 U76366 Treacher Collins syndrome (TCOF1); Also: U84665, U40847 −2.2445863000 M77829 Channel-like integral membrane protein (CHIP28); Also: S73482 1.8463279000 D63478 KIAA0144 −2.2079372000 U93049 SLP-76 associated protein 1.8208888000 M36542 Lymphoid-specific transcription factor; Also: X13810, X13809 −2.2043574000 HG3731-HT4001 Ig Heavy Chain, Vdjrc Regions L23566 1.8025389000 M95178 Non-muscle alpha-actinin 1.7921114000 X98225 Gastrin-binding protein/X98225 1.7825443000 X15306 NF-H 1 −2.1689075000 *M24766 Alpha-2 collagen type IV (COL4A2); Also: X05610 1.7779340000 X07834 Manganese superoxide dismutase SOD2 1.7802453000 D44466 Proteasome subunit p112 −2.1663931000 Z49254 L23-related −2.1637203000 U18550 GPR3 G protein-coupled receptor 1.7746994000 J05068 Transcobalamin I 1.7700047000 M59820 Granulocyte colony-stimulating factor receptor (CSF3R) 1.7714405000 U38480 Retinoid X receptor-gamma −2.1610684000 X87212 Cathepsin C 1.7590364000 HG2036-HT2090 Stimulatory Gdp/Gtp Exchange protein C-Ki-Ras P21/Smg P21 −2.1415673000 Y08409 Spot14 −2.1407044000 L47345 Elongin A −2.1360464000 U49837 LIM protein MLP −2.1346153000 M96944 B-cell specific TRANSCRIPTION FACTOR (BSAP) 1.7306208000 M98045 Folylpolyglutamate synthetase −2.1298107000 D80004 KIAA0182 −2.1272263000 X70991 MADER 1.7156601000 X64037 RNA polymerase II associated protein RAP74 −2.0997238000 U50360 Calcium, calmodulin-dependent protein kinase II gamma/U50360 −2.0863598000 J05257 Clones MDP4 MDP7 microsomal dipeptidase (MDP) 1.6624745000 U79261 Clone 23959; Also: U62317_rna1 −2.0810321000 X77588 HG3988-HT4258 and others −2.0753188000 X17094 Furin 1.6512295000 M13207 Granulocyte-macrophage colony-stimulating factor (CSF1) −2.0635210000 S85963 hIRS-1 = rat insulin receptor substrate-1 homolog 1.6198012000 *X57809 Rearranged Ig lambda light chain; Also: S42404 1.6185978000 U49260 Mevalonate pyrophosphate decarboxylase (MPD) −2.0366788000 D42040 KIAA9001; Also: X62083, M80613 −2.0292924000 U62293 LIMK1 (LIM-kinase1); Also: U63721_rna2, U63721_rna2 −2.0282153000 HG491-HT491 Fc Receptor lib3 For Igg, Low Affinity 1.6060050000 HG2797-HT2906 Clathrin, Light Polypeptide B-Also: X81637, HG2797-HT2905 −2.0267375000 M25322 Granule membrane protein-140 −2.0059844000 X06956 HALPHA44 alpha-tubulin −2.0045900000 D29642 KIAA0053 1.5838220000 Y00970 Acrosin (EC 342110) 1.5839352000 *S82024 SCG10 = neuron-specific growth-associated protein −1.9997722000 D83920 Uterus ficolin-1 1.5799550000 U47621 Nucleolar autoantigen No55 1.5800958000 M85247 Dopamine D1A receptor/M85247 −1.9920009000 U37219 Cyclophilin-like protein CyP-60 −1.9864918000 **X05299 (˜95%) major centromere autoantigen CENP-B 1.5698259000 X63380 RSRFR2 1.5688006000 AF002224 E6-AP ubiquitin protein ligase 3A/promoter P1 1.5625902000 HG2348-HT2444 Peptide Yy; Also: D13897_rna2 1.5661874000 HG2259-HT2348 Tubulin, Alpha 1; Also: X06956 −1.9746844000 M36200 Synaptobrevin 1 (SYB1) −1.9770946000 M13981 Inhibin A-subunit 1.5621968000 D13636 KIAA0011 −1.9620140000 U68031 G protein-coupled receptor (STRL22)/U68031 1.5521813000 Z38133 Myosin; Also: M36769 1.5518470000 M80647 Thromboxane synthase 1.5441298000 X14474 Microtubule-associated tau protein 1.5436335000 X14813 3-oxoacyl-CoA thiolase −1.9496339000 HG1728-HT1734 CGM1 1.5412047000 L35240 Enigma 1.5380079000 HG1098-HT1098 Cystatin D 1.5345338000 L42176 (clone 353) DRAL 1.5358003000 S66431 RBP2 = retinoblastoma binding protein 2 1.5358003000 U58090 Hs-cul-4A 1.5331363000 X51954 UCP1 uncoupling protein/X51954 1.5328482000 HG4593-HT4998 Sodium Channel 1 −1.9391106000 U17886 Succinate dehydrogenase iron-protein subunit (sdhB) −1.9363881000 U37519 Aldehyde dehydrogenase (ALDH8) −1.9341827000 D84557 HsMcm6 −1.9302484000 M62843 Antigen in paraneoplastic sensory neuronopathy patients −1.9305033000 L10377 (clone CTG-B37) sequence; Also: D38529, U23851, D31840 1.5271786000 HG2825-HT2949 Ret Transforming −1.9244085000 L10717 T cell-specific tyrosine kinase 1.5193028000 M25897 Platelet factor 4 (PF4) 1.5222276000 U85265 Down syndrome critical region 1 (DSCR1) alternative 1 1.5216642000 D10995 Serotonin 1B receptor −1.9209056000 X52008 Strychnine binding subunit of inhibitory glycine receptor −1.9199275000 HG3491-HT3685 Zinc Finger protein Zfp-36 1.5150123000 U20647 Zinc finger protein (ZNF151) −1.9093554000 L77213 Phosphomevalonate kinase −1.9056610000 S82240 RhoE = 26 kda GTPase homolog 1.5021539000 *M74826 Glutamate decarboxylase (GAD-2) −1.8953535000 *X07109 Protein kinase C (PKC) type beta II −1.8952153000 HG4490-HT4876 Proline-Rich protein Prb4, Allele −1.8905607000 HG4051-HT4321 Choline Acetyltransferase 1.4882686000 M21665 Beta-myosin heavy chain; Also: X52889 1.4892253000 X81420 hHKb1 protein 1.4919523000 L23333 Corticotropin releasing factor receptor; Also: X72304 −1.8873359000 D16815 EAR-1r 1.4869969000 M25280 Lymph node homing receptor 1.4825163000 D43968 AML1b protein −1.8803133000 K03183 Chorionic gonadotropin beta subunit −1.8803276000 M13232 Factor VII serine protease precursor; Also: J02933 −1.8815986000 U23803 Heterogeneous ribonucleoprotein A0 −1.8788827000 U59736 TRANSCRIPTION FACTOR (NFATcb) −1.8802368000 L09708 Complement component 2 (C2) allele b 1.4794162000 X78992 ERF-2 1.4819119000 X80026 B-cam −1.8752784000 Y07755 S100A2 −1.8752784000 HG2709-HT2805 Serine/Threonine Kinase 1.4744348000 L40396 (clone s22i71) 1.4763968000 D83784 KIAA0198 −1.8699647000 L13972 Beta-galactoside alpha-23-sialyltransferase (SIAT4A) −1.8688648000 X16667 HOX2G from the Hox2 locus −1.8693784000 U24577 LDL-phospholipase A2 1.4699388000 L41147 5-HT6 serotonin receptor −1.8659918000 U31929 Orphan nuclear receptor (DAX1); Also: S74720 −1.8651780000 U79271 Clones 23920 and 23921 sequence 1.4633207000 U96131 HPV16 E1 protein binding protein/U96131 −1.8599635000 D59253 NCBP interacting protein 1 1.4611983000 J04102 Erythroblastosis virus onco homolog 2 (ets-2) 1.4614809000 X68149 BLR1 Burkitt's lymphoma receptor 1 1.4621733000 AF001620 Trabecular meshwork-induced glucocorticoid response protein 1.4517097000 S77763 Nuclear factor erythroid 2 isom f = basic leucine zipper protein −1.8464144000 L20826 I-plastin −1.8419067000 U60415 bHLH-PAS protein Jap3 1.4420092000 X06389 Synaptophysin (p38) 1.4336098000 X17360 HOX 5.1 protein 1.4333697000 M97496 Guanylin 1.4266739000 S81578 Dioxin-responsive/S81578 1.4274050000 U80017 Survival motor neuron protein 1.4251371000 X67318 Procarboxypeptidase A1 1.4263486000 M60299 Alpha-1 collagen type II s 1 2 and 3/M60299 −1.8246952000 D85939 p97 homolog 1.4219328000 M22403 Blood platelet membrane glycoprotein Ib-alpha (GPIB) 1.4189234000 X99296 RD/X99296 1.4203205000 M73481 Gastrin releasing peptide receptor (GRPR) −1.8188030000 U53476 Proto-onco Wnt7a −1.8187206000 D42045 KIAA0086 1.4135512000 M12759 Ig J chain 1.4128674000 S71043 Ig alpha 2 = Ig A heavy chain allotype 2; Also: S55735 1.4131120000 X14690 Plasma inter-alpha-trypsin inhibitor heavy chain H(3) 1.4075608000 X74039 Urokinase plasminogen activator receptor −1.8169866000 X87904 SEP protein −1.8142476000 X90840 Axonal transporter of synaptic vesicles −1.8153287000 M63256 Major Yo paraneoplastic antigen (CDR2) 1.4072771000 U20240 C/EBP gamma 1.4061322000 M16707 Histone H4; clone FO108 −1.8076683000 X54871 Ras-related protein Rab5b 1.3981137000 S72493 Keratin = keratin 16 homolog; Also: M28439 −1.8036278000 U68233 Farnesol receptor HRR-1 (HRR-1) −1.8026027000 X74794 P1-Cdc21 −1.8037791000 X87871 Hepatocyte nuclear factor 4b; Also: X87870, Z49825 −1.8050759000 Z84721 DNA from 16p13.3 Contains alpha and zeta globin −1.8031156000 M68516 PCI (plasminogen activator inhibitor 3) from protein C inhibitor 1.3888114000 U46746 Dystrobrevin-epsilon; Also: U46744 1.3918125000 S68874 EP3 prostanoid receptor EP3-I; Also: D86096_1, X83858 −1.8020036000 X89211 DNA endogenous retroviral like element/X89211 −1.7982189000 HG3570-HT3773 Protein Phosphatase Inhibitor Homolog −1.7935634000 X63755 High-sulphur keratin 1.3680604000 L08424 Achaete scute homologous protein (ASH1) −1.7847064000 D86062 KNP-Ib; Also: U53003 1.3634666000 M95929 Homeobox protein (PHOX1) 1.3627651000 S75313 MJD1 = MJD1 protein {CAG repeats} 1.3585874000 X70649 CI1042 of DEAD box protein family −1.7784226000 Y00757 Polypeptide 7B2 −1.7792698000 D87002 POM121-like 1 1.3552599000 HG2260-HT2349 Duchenne Muscular Dystrophy protein (Dmd); Also: M18533 1.3538201000 M25809 Endomembrane proton pump subunit −1.7725967000 X62515 Basement membrane heparan sulfate proteoglycan −1.7758834000 U22662 Nuclear orphan receptor LXR-alpha 1.3447851000 D79998 KIAA0176 −1.7700231000 HG919-HT919 Dna Polymerase Epsilon Catalytic Subunit −1.7714956000 J05252 Also: M95971 −1.7686381000 U96629 Hereditary multiple exostosis 1.3424227000 M74093 Cyclin −1.7639892000 S79781 WT1/S79781 −1.7641855000 M55024 Cell surface glycoprotein P3.58;/M55024; Also: M24283 1.3357587000 U09550 Oviductal glycoprotein 1.3283163000 D26561 ORF E7 from papillomavirus 5b genome −1.7600453000 M97252 Kallmann syndrome (KAL) 1.3249620000 D17516 PACAP receptor 1.3201401000 D49493 Bone morphogenetic protein-3b 1.3221159000 L02867 62 kDa paraneoplastic antigen −1.7546350000 M34539 FK506-binding protein (FKBP) −1.7572062000 M17183 Parathyroid hormone-related protein; Also: M24351_3, J03580 1.3152354000 D87937 Alpha(1,2)fucosyltransferase 5 −1.7500260000 D89377 MSX-2 −1.7507012000 U43843 H-neuro-d4 protein −1.7503155000 D42054 KIAA0092 1.3057652000 M55905 Mitochondrial NAD(P)+ dependent malic enzyme 1.3051620000 U28281 secretin receptor −1.7464396000 Z34975 LDLC −1.7474409000 HG3187-HT3366 Tyrosine Phosphatase 1; Also: HG3187-HT3365, U12128 1.3023642000 M27543 Guanine nucleotide-binding protein (Gi) alpha subunit 1.3007215000 U18991 Retinal pigment epithelium-specific 61 kDa protein (RPE65) 1.2986348000 HG4245-HT4515 Khead Family Afx1 1.2941354000 M83652 Complement component properdin; Also: X57748 1.2929203000 HG4234-HT4504 Methylenetetrahydrofolate Reductase −1.7398689000 Z74792 CCAAT transcription binding factor subunit gamma −1.7387806000 S66896 Squamous cell carcinoma antigen = serine protease inhibitor 1.2912578000 D17400 6-pyruvoyl-tetrahydropterin synthase −1.7353993000 Y08134 ASM-like phosphodiesterase 3b −1.7374908000 D29992 Placental protein 5 (PP5) 1.2797753000 X15088 GNAT1 transducin alpha-chain 1.2820442000 HG1747-HT1764 Proto-Oncogene Met; Also: J02958, U08818 −1.7316895000 M12886 T-cell receptor active beta-chain −1.7301764000 U07231 G-rich sequence factor-1 (GRSF-1) −1.7299743000 X17254 TRANSCRIPTION FACTOR Eryf1 −1.7314880000 X77567 InsP3 5-phosphatase; Also: Z31695 1.2761490000 V00535 IFNB 1; Also: J00218_rna1, V00547, M28622, V00534_rna1 1.2694863000 L22454 Nuclear respiratory factor-1 (NRF-1) −1.7246854000 M18700 D00306, M16630, M18692 −1.7273379000 U79245 Clone 23586 sequence −1.7266253000 X02404 CGRP from medullary thyroid carcinoma (MTC) −1.7271344000 Z46376 HK2 hexokinase II 1.2635177000 D14134 RAD51 1.2598327000 U79293 Clone 23948 sequence 1.2617385000 L21998 Intestinal mucin (MUC2) −1.7202627000 M65062 Insulin-like growth factor binding protein 5 (IGFBP-5) 1.2530956000 U78095 Placental bikunin −1.7129652000 D10495 Protein kinase C delta-type 1.2435668000 HG3288-HT3465 Xanthine Dehydrogenase −1.7119126000 M21984 (clone PWHTnT16) skeletal muscle Troponin T −1.7104347000 U47928 Protein A alternatively spliced m 2 (A-2) −1.7110687000 X52228 Secreted epithelial tumor mucin antigen −1.7084421000 X59373 HOX4D a homeobox protein −1.7115964000 HG2841-HT2969 Albumin, 3; Also: HG2841-HT2970, HG2841-HT2968 1.2377036000 U29589 m3 muscarinic acetylcholine receptor (CHRM3) 1.2402996000

[0028] TABLE 4 Gene targets in MS spinal cord gray matter from a sample with axonal loss. Probe set Gene description log10 (ratio) fold change D26129 RNase A −2.7780879000 *M87789 Anti-hepatitis A IgG V, C, CDR regions; Also: J00221_2 3.7091911000 *M63438 Ig rearranged gamma chain, V-J-C region; Also: X96754 3.6640039000 L13210 Mac-2 binding protein −2.6950437000 L16862 G protein-coupled receptor kinase (GRK6) −2.6041720000 M25280 Lymph node homing receptor 2.0987648000 D49357 S-adenosylmethionine synthetase 2.0759381000 L76200 Guanylate kinase (GUK1) −2.5051160000 X74570 Gal-beta(1-3/1-4)GlcNAc alpha-23-sialyltransferase −2.4956310000 S68616 Na+/H+ exchanger NHE-1 isom −2.4902746000 L44140 DNL1L from chromosome X region; Also: X90392 2.0235817000 L14565 Peripherin (PRPH) s 1-9 −2.4614422000 S76638 p50-NF-kappa B homolog 1.9947998000 HG2709-HT2805 Serine/Threonine Kinase 1.9764875000 X84213 BAK BCI-2 homolog; Also: U16811, U23765 1.9659539000 *X63578 Parvalbumin −2.3866104000 X14474 Microtubule-associated tau protein 1.9417846000 *D90086 Pyruvate dehydrogenase beta subunit −2.3701197000 L41143 Expressed pseudo TCTA at t(1;3) translocation site −2.3607117000 M63573 Secreted cyclophilin-like protein (SCYLP) 1.9226736000 *X64072 CD18; Also: M15395 1.9213222000 Z22548 Thiol-specific antioxidant protein −2.3496417000 M72885 GOS2; Also: M69199_rna1 1.9171115000 HG1067-HT1067 Mucin/M22406 1.9114934000 M80397 DNA polymerase delta catalytic subunit; Also: M81735 −2.3239221000 M22632 Mitochondrial aspartate aminotransferase −2.3186893000 *X00734 Beta-tubulin (5-beta) with ten Alu family members −2.2901738000 J04501 Muscle glycogen synthase 1.8619822000 L13266 N-methyl-d-aspartate receptor (NR1-1) −2.2750809000 D16583 L-histidine decarboxylase 1.8302678000 X87212 Cathepsin C 1.8308174000 U76366 Treacher Collins syndrome (TCOF1); Also: U84665, U40847 −2.2445863000 X69433 Mitochondrial isocitrate dehydrogenase (NADP+) −2.2474823000 Z29331 (23k/3) ubiquitin-conjugating enzyme UbcH2 1.8159097000 D63487 KIAA0153 −2.2291697000 U73799 Dynactin/U73799 1.7998573000 D12625 Neurofibromin 1.7918309000 D82348 Aminoimidazole carboxamide ribo-nt transmylase/inosinicase −2.2076344000 M36542 Lymphoid-specific transcription factor; Also: X13810, X13809 −2.2043574000 M21665 Beta-myosin heavy chain; Also: X52889 1.7723363000 U89336 Notch 4 −2.1940632000 J04132 T cell receptor zeta-chain 1.7635777000 U79271 Clones 23920 and 23921 sequence 1.7502416000 AC000099 Cosmid g0771a003 −2.1675758000 D90276 CGM7 nonspecific cross-reacting antigen (NCA) −2.1670957000 HG3995-HT4265 Cpg-Enriched Dna Clone S19 −2.1596800000 AF002224 E6-AP ubiquitin protein ligase 3A/promoter P1 1.7346798000 X67325 p27 −2.1546522000 L32137 Germline oligomeric matrix protein (COMP) 1.7239480000 Z46632 HSPDE4C1 3,5-cyclic AMP phosphodiesterase 1.7264012000 Y08409 Spot14 −2.1407044000 U56976 Calmodulin dependent phosphodiesterase PDE1B1 1.7128601000 X04145 T-cell receptor T3 gamma polypeptide 1.7165042000 M13755 Interferon-induced 17-kDa/15-kDa protein −2.1362051000 S66431 RBP2 = retinoblastoma binding protein 2 1.7037212000 M98045 Folylpolyglutamate synthetase −2.1298107000 U47621 Nucleolar autoantigen No55 1.6981708000 X57351 1-8D from interferon-inducible family −2.1186367000 HG491-HT491 Fc Receptor lib3 For lgg, Low Affinity 1.6904619000 X89986 NBK apoptotic inducer protein; Also: U49730, U34584 1.6868596000 HG3987-HT4257 Cpg-Enriched Dna Clone E06 −2.1094182000 AD000684 LISCH7 (liver-specific bHLH-Zip transcription factor) 1.6814222000 **X05299 (˜95%) major centromere autoantigen CENP-B 1.6791289000 AF001294 IPL −2.1022192000 U50743 NaK-ATPase gamma subunit −2.0976043000 M65085 Follicle stimulating hormone receptor 1.6673862000 M35252 CO-029 −2.0848443000 L36463 Ras inhibitor (Rin1) 1.6544690000 U79261 Clone 23959; Also: U62317_rna1 −2.0810321000 X99142 Hair keratin hHb6 −2.0812573000 HG3991-HT4261 Cpg-Enriched Dna, Clone E18 1.6428106000 U13369 Ribosomal DNA repeating unit/U13369 1.6399345000 U46746 Dystrobrevin-epsilon; Also: U46744 1.6422686000 M13207 Granulocyte-macrophage colony-stimulating factor (CSF1) −2.0635210000 X69838 G9a −2.0635210000 Z22555 Encoding CLA-1 −2.0576186000 Z33905 43 kD acetylcholine receptor-associated protein (Rapsyn) 1.6197193000 U39573 Salivary peroxidase −2.0552349000 J03600 Lipoxygenase −2.0488301000 Y00757 Polypeptide 7B2 −2.0487933000 L13698 Growth-arrest-specific protein (gas) 1.6115584000 U22662 Nuclear orphan receptor LXR-alpha 1.6076694000 X17360 HOX 5.1 protein 1.6118826000 Z38133 Myosin; Also: M36769 1.6092717000 X70991 MADER 1.6063349000 M13981 Inhibin A-subunit 1.6011419000 U49260 Mevalonate pyrophosphate decarboxylase (MPD) −2.0366788000 AF009674 Axin 1.5857071000 U91316 Acyl-CoA thioester hydrolase −2.0287237000 D86971 KIAA0217 1.5813868000 HG2797-HT2906 Clathrin, Light Polypeptide B- Also: X81637, HG2797-HT2905 −2.0267375000 M16707 Histone H4; clone FO108. −2.0251522000 D50923 KIAA0133 1.5725231000 S69369 PAX3A = TRANSCRIPTION FACTOR 1.5694910000 M63582 Preprothyrotropin-releasing hormone −2.0136797000 D49493 Bone morphogenetic protein-3b 1.5591882000 AC002115 COX6B −2.0121515000 X98833 Zinc finger protein, Hsal1 −2.0089194000 D50532 Macrophage lectin 2 1.5516018000 D50913 KIAA0123 −2.0061450000 M25322 Granule membrane protein-140 −2.0059844000 M33882 p78 protein −2.0057702000 X06956 HALPHA44 alpha-tubulin −2.0045900000 M64231 Spermidine synthase −1.9982048000 HG3748-HT4018 Basic Transcription Factor 44 Kda Subunit 1.5370001000 K03021 Tissue plasminogen activator (PLAT) −1.9892829000 Z14244 CoxVIIb cytochrome c oxidase subunit VIIb −1.9903944000 U37219 cyclophilin-like protein CyP-60 −1.9864918000 D50402 NRAMP1 1.5099211000 HG2259-HT2348 Tubulin, Alpha 1; Also: X06956 −1.9746844000 HG2463-HT2559 Guanine Nucleotide-Binding protein G25k −1.9741085000 X04201 Skeletal muscle tropomyosin −1.9737627000 X97630 Serine threonine protein kinase EMK −1.9752020000 J00220 IGHA1 from Ig germline H-chain G-E-A region A: gamma-3 5 1.4976974000 L76568 S26 from excision and cross link repair protein ERCC4/L76568 −1.9693577000 M96944 B-cell specific TRANSCRIPTION FACTOR (BSAP) 1.4969988000 U01828 Microtubule-associated protein 2 (MAP2) 1.4951973000 U96629 Hereditary multiple exostosis 1.4901693000 M60298 Erythrocyte membrane protein band 42 (EPB42) 1.4847268000 *U89606 Pyridoxal kinase 1.4845845000 U22970 16-Jun (interferon-inducible peptide precursor) −1.9576671000 U01157 Glucagon-like peptide-1 receptor with CA dinucleotide repeat 1.4775752000 X16282 Zinc finger protein (clone 647) 1.4782778000 X81851 IL-4 splice variant/X81851; Also: M13982 1.4752438000 U25988 Pregnancy-specific glycoprotein 13 (PSG1) −1.9489628000 X71490 Vacuolar proton ATPase subunit D −1.9519443000 X05908 Lipocortin 1.4691078000 D86956 KIAA0201 1.4661771000 X13589 Aromatase (estrogen synthetase) 1.4643405000 Z14093 Branched chain decarboxylase alpha subunit 1.4654723000 *M85220 Heavy chain disease IgA chain CH3 region 1.4526297000 U02031 Sterol regulatory element binding protein-2 1.4533794000 L21993 Adenylyl cyclase 1.4503590000 D84454 UDP-galactose translocator 1.4436628000 U20240 C/EBP gamma 1.4431197000 D84557 HsMcm6 −1.9302484000 M62843 Antigen of paraneoplastic sensory neuronopathy patients −1.9305033000 U65676 Hermansky-Pudlak syndrome protein (HPS) 1.4405943000 Z22780 Cylicin 1.4387218000 X89101 Fas (Apo-1, CD95)/X89101; Also: X83493, X63717, X83492 −1.9231144000 L25444 TAFII70-alpha −1.9207102000 X52008 Strychnine binding subunit of inhibitory glycine receptor −1.9199275000 *M58459 Ribosomal protein (RPS4Y) isom −1.9165197000 U78525 Eukaryotic translation initiation factor (elF3) −1.9140786000 X52611 Transcription factor AP-2; Also: HG2465-HT4871, M36711 −1.9158613000 U60415 bHLH-PAS protein Jap3 1.4213571000 AF000545 Putative purinergic receptor P2Y10 −1.9043097000 *M35999 Platelet glycoprotein IIIa (GPIIIa) 1.4089180000 X07743 Pleckstrin (P47) 1.4044376000 X56687 Autoantigen NOR-90; Also: X53461, X53390, U65487_rna1 −1.8983823000 M87507 Interleukin-1 beta convertase (IL1BCE); Also: U13697 1.4005185000 U83598 Death domain receptor 3 soluble form (DDR3); Also: U94512 −1.8947313000 *X07109 Protein kinase C (PKC) type beta II −1.8952153000 M76446 Alpha-A1-adrenergic receptor 1.3928727000 D38498 PMS5 (yeast PMS1 homolog) −1.8904909000 U64998 Ribonuclease k6 precursor/U64998 1.3909219000 U91327 Chromosome 12p15 BAG clone CIT987SK-99D8 sequence 1.3911998000 U18235 ATP-binding cassette protein (ABC2) HFBCD04 clone 1.3866834000 U18919 Chromosome 17q12-21 clone pOV-2 1.3860456000 L19183 MAC30 −1.8868431000 D43968 AML1b protein −1.8803133000 M94065 Dihydroorotate dehydrogenase −1.8800272000 U38268 Cytochrome b pseudo/U38268 −1.8799556000 U61262 Neogenin −1.8810992000 U87964 Putative G-protein (GP-1) −1.8814560000 L48692 (clone p5-23-3) 1.3767594000 HG167-HT167 Hypothetical protein Npiiy20/M76676 1.3646448000 J04449 (clone NF 10) cytochrome P-450 nifedipine oxidase 1.3637999000 D83784 KIAA0198 −1.8699647000 X16667 HOX2G from the Hox2 locus −1.8693784000 HG2755-HT2862 T-Plastin −1.8637688000 U96094 Sarcolipin (SLN) −1.8651040000 X01038 Fetal apolipoprotein AI precursor; Also: X07496, X00566 −1.8629658000 X77794 Cyclin G1 −1.8655481000 HG2992-HT5186 Beta-Hexosaminidase Alpha Polypeptide 1.3552284000 L09708 Complement component 2 (C2) allele b 1.3547290000 M24486 Prolyl 4-hydroxylase alpha subunit; Also: M24487, U14620_1 1.3536952000 U27699 PephBGT-1 betaine-GABA transporter 1.3549090000 Z34974 Plakophilin; Also: X79293 1.3510229000 D82061 Short-chain alcohol dehydrogenase family −1.8595886000 D84361 p52 and p64 N-Shc −1.8598285000 U64197 Chemokine exodus −1.8589881000 M58460 75-kD autoantigen (PM-Sc1) 1.3408405000 U28749 High-mobility group phosphoprotein isoform I-C (HMGIC) 1.3392448000 U49973 Tigger 1 transposable element 1.3372595000 *D84145 WS-3 −1.8500333000 HG982-HT982 Pre-T/Nk-Cell-Associated protein 1f6; Also: L17326 −1.8476498000 X62078 GM2 activator protein −1.8455631000 M19684 Alpha-1-antitrypsin-related protein 1.3239736000 U51003 DLX-2 (DIx2); Also: L07919 1.3250466000 M15169 Beta-2-adrenergic receptor 1.3215725000 M22403 Blood platelet membrane glycoprotein lb-alpha (GPIB) 1.3166020000 U43916 Tumor-associated membrane protein homolog (TMP) 1.3161801000 D16581 8-oxo-dGTPase −1.8333200000 U00946 Clone A9A2BRB5 (CAC)n/(GTG)n repeat-containing 1.3119428000 *U62317 Hypothetical protein 384D8_7 1.3095598000 HG2707-HT2803 Serine/Threonine Kinase 1.3074800000 L75847 Zinc finger protein 45 (ZNF45) 1.3063484000 AF001548 815A9.1 myosin heavy chain from chromosome 16 BAC −1.8301883000 M59916 Acid sphingomyelinase (ASM) −1.8284988000 S75578 4-aminobutyrate aminotransferase/S75578; Also: L32961 −1.8297861000 M83822 Beige-like protein (BGL) 1.3001886000 M96132 MHC class II HLA-DR-beta-1*09012 (HLA-DRB1*09012) 1.3008128000 J02943 Corticosteroid binding globulin −1.8248577000 M60299 Alpha-1 collagen type II s 1 2 and 3/M60299 −1.8246952000 HG3088-HT3263 Splicing Factor Sc35 m 3 1.2950756000 X78925 HZF2 zinc finger protein 1.2900346000 M73481 Gastrin releasing peptide receptor (GRPR) −1.8188030000 L11931 Cytosolic serine hydroxymethyltransferase (SHMT) 1.2870175000 X60487 H4/h H4 histone 1.2873538000 U38964 PMS2 related (hPMSR2); Also: D38502 −1.8154117000 M17183 Parathyroid hormone-related protein; Also: M24351_3, J03580 1.2785250000 D85433 MURR1 −1.8097280000 Z48481 Membrane type matrix metalloproteinase 1 −1.8082110000 M87860 S-lac lectin L-14-II (LGALS2) 1.2683541000 L32866 Effector cell protease receptor-1 (EPR-1) −1.8044802000 M11726 Pancreatic polypeptide −1.8053309000 Z84721 DNA from 16p13.3 Contains alpha and zeta globin −1.8031156000 S58733 pp52 = B lymphocyte signal transduction 1.2642308000 D14446 HFREP-1 −1.7990820000 D37931 RNase4 −1.8018323000 *M11749 Thy-1 glycoprotein −1.7987879000 U01120 Glucose-6-phosphatase −1.7976137000 HG3570-HT3773 Protein Phosphatase Inhibitor Homolog −1.7935634000 Z72499 Herpesvirus associated ubiquitin-specific protease (HAUSP) −1.7969211000 U28488 Putative G protein-coupled receptor (AZ3B); Also: U62027 1.2483725000 U20860 Angiotensin II type 2 receptor 1.2451424000 L00205 K6b epidermal keratin type II −1.7875490000 S74683 ADP-ribosyltransferase −1.7919537000 U63336 MHC Class I region proline rich protein −1.7902852000 HG896-HT896 Thrombospondin 2 1.2414220000 M27878 DNA binding protein (HPF2) 1.2395497000 U39226 Myosin VIIA (USH1B) 1.2376463000 X79510 Protein-tyrosine-phosphatase D1 1.2361010000 L08424 Achaete scute homologous protein (ASH1) −1.7847064000 HG2614-HT2710 Collagen Type Viii Alpha 1 1.2321764000 Z70218 MN1 protein (clone ICRFp507I0498); Also: X82209 1.2278215000 U59228 Ectodermal dysplasia protein (EDA) −1.7784226000 U44848 Nuclear respiratory factor 1 (NRF1)/U44848/ 1.2209368000 HG3242-HT3419 Calcium Channel, Voltage-Gated, Alpha 1e Subunit, 2 −1.7753767000 M25809 Endomembrane proton pump subunit −1.7725967000 M27318 Interferon (IFN-alpha-M1) 1.2139137000 X51757 Heat-shock protein HSP70B′ 1.2104790000 X99350 HFH4 1.2102298000 Y08564 GalNAc-T4/Y08564 1.2076344000 HG4258-HT4528 Kinase Inhibitor P27kip1 Cyclin-Dependent −1.7678976000 HG919-HT919 Dna Polymerase Epsilon Catalytic Subunit −1.7714956000 D83920 Uterus ficolin-1 1.2042557000 M62505 C5a anaphylatoxin receptor 1.2027830000 Y08766 Splicing factor, SF1-Bo isoform; Also: L49380 1.2049504000 M32334 Intercellular adhesion molecule 2 (ICAM-2) −1.7634280000 S79781 WT1/S79781 −1.7641855000 X54380 Pregnancy zone protein 1.1975562000

[0029] TABLE 5 Gene targets in MS spinal cord white matter from a sample with minimal to no inflammation. Probe set Gene description log10 (ratio) fold change M84739 Autoantigen calreticulin 2.9768541000 M13755 Interferon-induced 17-kDa/15-kDa protein −2.6319001000 M29194 Triglyceride lipase 2.7169627000 M77829 Channel-like integral membrane protein (CHIP28); Also: S73482 2.6933453000 AF001359 Mismatch repair protein (hMLH1)/AF001359 −2.4844422000 X95876 G-protein coupled receptor −2.4699324000 AB000896 Cadherin FIB2 −2.4188397000 L48513 Paraoxonase 2 (PON2) −2.4034637000 M21904 4F2 glycosylated heavy chain (4F2HC) antigen 2.5422028000 D49818 Fructose 6-phosphate 2-kinase/fructose 2 6-bisphosphatase 2.5278232000 X00734 Beta-tubulin (5-beta) with ten Alu family members 2.5225746000 ***D16480 Mitochondrial enoylCoA hydratase 2.4726833000 M96326 Azurocidin −2.3481101000 U35234 Protein tyrosine phosphatase sigma 2.4405943000 M65066 cAMP-dependent protein kinase regulatory subunit RI-beta −2.3362095000 X86401 L-arginine: glycine amidinotransferase 2.4148938000 AB000895 Cadherin FIB1 −2.3181155000 D87433 KIAA0246 −2.3191061000 U45328 Ubiquitin-conjugating enzyme (UBE2I); Also: U31882, U66867 2.3617749000 D50863 TESK1 −2.2965007000 *D61391 Phosphoribosypyrophosphate synthetase-associated protein 39 −2.2951821000 HG3945-HT4215 Phospholipid Transfer protein 2.3041673000 AD000092 RAD23A homolog −2.2698630000 M60299 Alpha-1 collagen type II s 1 2 and 3/M60299 2.2705624000 U37219 Cyclophilin-like protein CyP-60 −2.2589364000 M90299 Glucokinase (GCK) −2.2545481000 L24774 Delta3, delta2-CoA-isomerase; Also: Z25821_rna1 Z25820 2.2454882000 D43968 AML 1b protein −2.2463139000 M63573 Secreted cyclophilin-like protein (SCYLP) 2.2362475000 U12707 Wiskott-Aldrich syndrome protein (WASP); Also: U19927 2.2370408000 D63486 KIAA0152 2.2290416000 D15049 Protein tyrosine phosphatase −2.2322971000 M96684 Pur (pur-alpha) 2.2042557000 J02947 Extracellular-superoxide dismutase (SOD3) 2.1949304000 L05148 Protein tyrosine kinase related sequence −2.2048658000 M36429 Transducin beta-2 subunit; Also: M16538 2.1834122000 U66559 Anaplastic lymphoma kinase receptor −2.1918002000 X17651 Myf-4 myogenic determination factor −2.1869563000 K03189 Chorionic gonadotropin beta subunit 2.1595672000 L41067 NF-AT4c −2.1758016000 J04501 Muscle glycogen synthase 2.1481347000 S78085 PDCD2 = programmed cell death-2/Rp8 homolog −2.1691599000 X81372 Biphenyl hydrolase-related protein −2.1664301000 U03270 Centrin −2.1609185000 U24183 Phosphofructokinase (PFKM); Also: HG1849-HT1878 2.1302939000 J00268 Insulin; Also: V00565, X70508, L15440, M10039 −2.1558672000 D28423 Pre-splicing factor SRp20 2.1225435000 L76702 B56-delta 2.1264561000 M91585 Br140 2.1259690000 M57609 DNA-binding protein (GLI3) −2.1494501000 X15331 Phosphoribosylpyrophosphate synthetase subunit one 2.1215598000 L00205 K6b epidermal keratin type II −2.1467480000 L43579 (clone 110298)/L43579; Also: L43575 2.1151110000 D49490 Disulfide isomerase-related protein −2.1380657000 M31776 M25296 and others 2.1119343000 U23430 Cholecystokinin type A receptor (CCK-A); Also: L19315 2.1105897000 X04366 Calcium activated neutral protease large subunit (muCANP) −2.1371166000 D80003 KIAA0181 −2.1313780000 D14822 CBFA2T1 −2.1245042000 U82671 HSP1-A from cosmids from Xq28 2.0900816000 U40002 Hormone-sensitive lipase testicular isoform; Also: L11706 2.0870323000 Z48314 Apomucin; Also: U06711 2.0870712000 HG3242-HT4231 Calcium Channel, Voltage-Gated, Alpha 1e Subunit, 3 −2.1080574000 D30755 KIAA0113 −2.1044871000 U77968 Neuronal PAS1 (NPAS1) 2.0672569000 J02645 Translational initiation factor (elF-2) alpha subunit −2.0896402000 U49278 Putative DNA-binding protein −2.0898168000 L32866 Effector cell protease receptor-1 (EPR-1) −2.0857364000 X13810 OTF-2 lymphoid-specific transcription factor; Also: M36542 −2.0805363000 U15131 p126(ST5) 2.0398106000 D11094 MSS1 2.0364293000 AB000409 MNK1 −2.0695756000 S81737 Alpha 1 syntrophin; Also: U40571 2.0324173000 M58026 NB-1 2.0184925000 X13956 12S RNA induced by poly(rI) poly(rC) and Newcastle virus −2.0547088000 D28532 Renal Na+-dependent phosphate cotransporter −2.0486360000 X99142 Hair keratin hHb6 2.0111474000 U15655 Ets domain prot ERF 2.0045363000 U16031 TRANSCRIPTION FACTOR IL-4 Stat −2.0447357000 U78793 Folate receptor alpha (hFR)/U78793 −2.0437551000 HG4757-HT5207 Oncogene MII-Af4, Fusion Activated; Also: L13773 −2.0424771000 L38503 Glutathione S-transferase theta 2 (GSTT2) −2.0343276000 D13988 Rab GDI 1.9896722000 M96738 Somatostatin receptor subtype 3 (SSTR3); Also: Z86000 1.9881128000 U86759 Netrin-2 like protein (NTN2I); Also: U86758_rna1 1.9829493000 D84239 IgG Fc binding protein −2.0197392000 AF002224 E6-AP ubiquitin protein ligase 3A/promoter P1 1.9738203000 *M94250 Retinoic acid inducible factor (MK) 1.9708116000 X68688 ZNF33B; Also: D31763 −2.0095571000 M91083 DNA-binding protein (HRC1) 1.9637878000 L41143 Expressed pseudo TCTA at t(1;3) translocation site 1.9602033000 U08191 R kappa B; Also: X80878 1.9614211000 X54637 Tyk2 non-receptor protein tyrosine kinase 1.9566486000 D79998 KIAA0176 −1.9967305000 U71364 Serine protase inhibitor (P19) −1.9973864000 M32879 Steroid 11-beta-hydroxylase (CYP11B1) 1.9385197000 *U37408 CtBP 1.9400182000 X02958 Interferon alpha IFN-alpha 6 −1.9815921000 M15881 Uromodulin (Tamm-Horsfall glycoprotein) −1.9748570000 U85658 TRANSCRIPTION FACTOR ERF-1 −1.9673139000 X12517 U1 small nuclear RNP-specific C protein 1.9188164000 U78180 Sodium channel 2 (hBNaC2) −1.9604708000 M21984 (clone PWHTnT16) skeletal muscle Troponin T −1.9555675000 X16260 Inter-alpha-trypsin inhibitor subunit 3; Also: X69532_rna1 1.9103576000 X63380 RSRFR2 1.9033593000 M21389 Keratin type II (58 kD) −1.9454686000 U07919 Aldehyde dehydrogenase 6 −1.9452223000 X76942 U41740 and others −1.9463294000 X89101 Fas (Apo-1, CD95)/X89101; Also: X83493, X63717, X83492 −1.9459607000 J05582 Pancreatic mucin; Also: J05581 1.9006585000 M22919 Non-muscle myosin light chain MLC −1.9378939000 L08488 Inositol polyphosphate 1-phosphatase 1.8954482000 U68723 Checkpoint suppressor 1 1.8934843000 X82850 Thyroid transcript factor 1; Also: U43203, U33749 1.8945929000 M59916 Acid sphingomyelinase (ASM) 1.8904865000 X07315 PP15 (placental protein 15) 1.8901415000 X58298 lnterleukin-6-receptor; Also: M20566 1.8918161000 U37519 Aldehyde dehydrogenase (ALDH8) −1.9301847000 HG3884-HT4154 Homeotic protein Hpx-42 1.8873359000 **X05299 (˜95%) major centromere autoantigen CENP-B 1.8790959000 X13293 B-myb 1.8782345000 D79985 KIAA0163 −1.9194703000 J00220 IGHA1 from Ig germline H-chain G-E-A region A: gamma-3 5 1.8759989000 J03171 Interferon-alpha receptor (HuIFN-alpha-Rec) −1.9122221000 U44754 PSE-binding factor PTF gamma subunit −1.9075457000 U53442 p38Beta MAP kinase −1.9100905000 *X64072 CD18; Also: M15395 1.8668778000 M15465 Pyruvate kinase type L; Also: D13243 −1.9063350000 X87870 Hepatocyte nuclear factor 4a −1.9037680000 L43338 (clone JJ1a) cadherin/L43338 −1.8995469000 Z19002 PLZF kruppel-like zinc finger protein −1.8955607000 U89896 Casein kinase I gamma 2 1.8524800000 D45917 TIMP-3; Also: U14394 −1.8909796000 U06698 Neuronal kinesin heavy chain −1.8904210000 L02867 62 kDa paraneoplastic antigen 1.8457180000 M21302 Small proline rich protein (sprll), clone 174 N 1.8464883000 U60116 Skeletal muscle LIM-protein SLIM2 1.8438554000 X81420 hHKb1 protein 1.8452505000 AB002315 KIAA0317 −1.8874766000 D86971 KIAA0217 1.8337844000 L31881 Nuclear factor I-X 1.8360075000 X59303 G7a valyl-tRNA synthetase; Also: M98326 1.8369567000 U65011 Preferentially expressed antigen of melanoma (PRAME) −1.8787920000 Z71389 Skin-antimicrobial-peptide 1 (SAP1)/Z71389 −1.8800987000 U15932 Dual-specificity protein phosphatase −1.8727388000 X13766 Beta-casein; Also: L10615, X17070 −1.8754953000 X73079 Encoding Polymeric Ig receptor −1.8757845000 U50360 Calcium, calmodulin-dependent protein kinase II gamma/U50360 1.8249558000 AF009674 Axin −1.8701112000 M58297 Zinc finger protein 42 (MZF-1) −1.8720105000 U65093 Msg1-related 1 (mrg1) −1.8704039000 U83192 Post-synaptic density protein 95 (PSD95) 1.8185558000 J05614 Proliferating cell nuclear antigen (PCNA) promoter region 1.8165727000 *M63438 Ig rearranged gamma chain , V-J-C region; Also: X96754 1.8081860000 U96769 Chondroadherin 1.8027737000 U83843 HIV-1 Nef interacting protein (Nip7-1)/U83843 1.7996851000 HG3495-HT3689 Collagen Type Ix Alpha 1 −1.8500333000 L47276 (cell line HL-60) alpha topoisomerase/L47276; Also: L47277 −1.8492658000 *M85220 Heavy chain disease IgA chain CH3 region 1.7895246000 U26266 Deoxyhypusine synthase/U26266; Also: U79262 1.7888751000 U09366 Zinc finger protein ZNF133 −1.8413595000 U17743 JNK activating kinase (JNKK1); Also: L36870 −1.8407332000 Y08374 GP-39 cartilage protein −1.8399492000 U65404 Erythroid-specific TRANSCRIPTION FACTOR EKLF 1.7849737000 J02963 Platelet glycoprotein IIb −1.8363241000 M84820 Retinoid X receptor beta (RXR-beta); Also: X63522, X65463 −1.8347385000 Z35309 Adenylyl cyclase −1.8325089000 D87457 KIAA0281 1.7785130000 X74328 CB2 (peripheral) cannabinoid receptor 1.7792356000 X79483 ERK6 extracellular signal regulated kinase 1.7785130000 Z16411 Phospholipase c; Also: U26425, Z37544_rna1 1.7817554000 Z80345 SCAD; Also: M26393 1.7813963000 D49817 Fructose 6-phosphate 2-kinase/fructose 2 6-bisphosphatase 1.7767012000 X97444 Transmembrane protein Tmp21-IIex/X97444 1.7726884000 Y07566 RIT protein −1.8238002000 M36089 DNA-repair protein (XRCC1) 1.7723217000 X86018 MUF1 protein 1.7671559000 Y12478 CHD5 protein 1.7635395000 Z69881 Adenosine triphosphatase calcium −1.8223316000 X60655 EVX1 1.7558749000 D14686 Glycine cleavage system T-protein −1.8098962000 U01160 Transmembrane 4 superfamily protein (SAS) −1.8108715000 HG162-HT3165 Tyrosine Kinase Receptor Axl 2 1.7516639000 K02054 Gastrin-releasing peptide −1.8056707000 L00137 Growth hormone releasing factor −1.8029447000 V00565 Preproinsulin; Also: M10039 1.7431176000 U08989 Glutamate transporter −1.8019180000 U79280 Clone 23575 −1.8014895000 M38258 Retinoic acid receptor gamma 1 1.7359979000 X69115 ZNF37A zinc finger protein −1.7964009000 HG3033-HT3194 Spliceosomal protein Sap 62 1.7284743000 M23294 Beta-hexosaminidase beta-subunit (HEXB) 1.7275413000 X14830 Muscle acetylcholine receptor beta-subunit −1.7894044000 X98507 Myosin-I beta −1.7876376000 D87078 KIAA0235 1.7267272000 U08049 Peripheral myelin protein-22 (PMP22) non-coding 1A/U08049 −1.7837250000 U14910 RPE-retinal G protein-coupled receptor (rgr) −1.7830098000 U90547 Ro/SSA ribonucleoprotein homolog (RoRet) −1.7831887000 D28383 ATP synthase B chain 1.7185017000 U70732 Glutamate pyruvate transaminase (GPT) 1.7178323000 D10495 Protein kinase C delta-type 1.7168377000 L78833 Ifp35 from BRCA1, Rho7 and vatl 1.7155856000 M37457 Na+, K+-ATPase catalytic subunit alpha-III isoform 1.7147488000 U77846 Elastin −1.7806773000 U87972 NAD+-isocitrate dehydrogenase/U87972 −1.7804973000 U35113 Metastasis-associated mta1 1.7084209000 X07876 Irp prot (int-1 related protein) −1.7772455000 X90858 Uridine phosphorylase −1.7732377000 Y08682 Carnitine palmitoyltransferase I type I; Also: U62733, U62317 −1.7767012000 U20428 SNC19 sequence 1.7071442000 L41919 HIC-1 fragment −1.7691926000 M11186 Prepro-oxytocin-neurophysin I (OXT) −1.7693773000 X62535 Diacylglycerol kinase −1.7712199000 HG3523-HT4899 Proto-Oncogene C-Myc; Also: L00058, HG3523-HT4900 1.6980926000 X56687 Autoantigen NOR-90; Also: X53461, X53390, U65487_rna1 1.6998235000 J04449 (clone NF 10) cytochrome P-450 nifedipine oxidase −1.7654823000 L40386 DP-2; Also: U18422 1.6946052000 L37199 (clone cD24-1) Huntington's disease candidate regiont 1.6879746000 U52373 Serine/threonine kinase MNB (mnb); Also: D85759, D86550 1.6916708000 L18920 MAGE-2 −1.7604225000 *M87789 Hybridoma H210 anti-hepatitis A IgG V, C, CDR regions 1.6826464000 U40490 Nicotinamide nucleotide transhydrogenase 1.6852938000 L43964 (clone F-T03796) STM-2 −1.7531999000 X96753 Chondroitin sulfate proteoglycan (MCSP) −1.7562556000 D42053 KIAA0091 1.6794279000 HG3437-HT3628 Myelin Proteolipid protein; Also: M54927 1.6731273000 M21665 Beta-myosin heavy chain; Also: X52889 1.6762362000 M31169 Propionyl-CoA carboxylase beta-subunit/M31169 1.6720979000 AF005361 Importin alpha 6 −1.7435098000 M91196 DNA-binding protein −1.7448795000 U35139 NECDIN related protein 1.6669857000 M22324 Aminopeptidase N −1.7395723000 *M74826 Glutamate decarboxylase (GAD-2) −1.7407573000 X60957 Tie putative receptor tyrosine kinase −1.7393745000 HG4518-HT4921 Transcription Factor Btf3 Homolog M90355 1.6603911000

[0030] TABLE 6 Gene targets in MS spinal cord white matter from a sample with lymphocytic inflammation, demyelination and axonal loss. Probe set Gene description log10 (ratio) fold change *M63438 Ig rearranged gamma chain V-J-C region; Also: X96754 2.8860030000 AB000584 TGF-beta superfamily protein −2.9452516000 L00389 Cytochrome P-450 4 −2.9300826000 M84739 Autoantigen calreticulin 2.6676864000 M13755 Interferon-induced 17-kDa/15-kDa protein −2.6319001000 HG3945-HT4215 Phospholipid Transfer protein 2.4979657000 *M87789 Anti-hepatitis A IgG V, C, CDR regions; Also: J00221_2 2.4941391000 D26561 ORF E7 from papillomavirus 5b genome −2.4064124000 HG3033-HT3194 Spliceosomal protein Sap 62 2.4704774000 U22970 16-Jun (interferon-inducible peptide precursor) −2.3853381000 X93996 AFX protein 2.4455264000 M21904 4F2 glycosylated heavy chain (4F2HC) antigen 2.4151404000 AB000895 Cadherin FIB1 −2.3181155000 Y00757 Polypeptide 7B2 −2.3219607000 M96684 Pur (pur-alpha) 2.3033041000 D17716 N-acetylglucosaminyltransferase V −2.2915353000 M16653 Pancreatic elastase IIB −2.2924222000 HG3995-HT4265 Cpg-Enriched Dna Clone S19 −2.2683997000 D10495 Protein kinase C delta-type 2.2642273000 D63486 KIAA0152 2.2668195000 J04501 Muscle glycogen synthase 2.2589870000 U37219 Cyclophilin-like protein CyP-60 −2.2589364000 D43968 AML1b protein −2.2463139000 X67325 p27 −2.2399248000 U12707 Wiskott-Aldrich syndrome protein (WASP); Also: U19927 2.2246625000 *X64072 CD18; Also: M15395 2.2272438000 M33882 p78 protein −2.2166936000 U45328 Ubiquitin-conjugating enzyme (UBE2I); Also: U31882 2.1997661000 U40279 Beta-2 integrin alphaD subunit (ITGAD)/U40279 −2.1967977000 X53683 LAG-1 −2.1972116000 *X13334 CD14 myeloid cell-specific leucine-rich glycoprotein 2.1776808000 L41143 Expressed pseudo TCTA at t(1; 3) translocation site 2.1658892000 U87964 Putative G-protein (GP-1) −2.1662080000 M63573 Secreted cyclophilin-like protein (SCYLP) 2.1523334000 HG3987-HT4257 Cpg-Enriched Dna Clone E06 −2.1621161000 L00205 K6b epidermal keratin type II −2.1467480000 X95406 Cyclin E −2.1339379000 M77829 Channel-like integral membrane protein (CHIP28) 2.1191604000 M61199 Cleavage signal 1 protein 2.1075491000 U82310 Unknown protein/U82310 −2.1044871000 M28825 Thymocyte antigen CD1a −2.0982975000 U15655 Ets domain protein ERF 2.0989896000 M23294 Beta-hexosaminidase beta-subunit (HEXB) 2.0948204000 L32866 Effector cell protease receptor-1 (EPR-1) −2.0857364000 K03189 Chorionic gonadotropin beta subunit 2.0920185000 L76702 B56-delta 2.0888446000 X13810 OTF-2 lymphoid-specific transcription factor; Also: M36542 −2.0805363000 J02947 Extracellular-superoxide dismutase (SOD3) 2.0849336000 D50402 NRAMP1 2.0795430000 X54637 Tyk2 non-receptor protein tyrosine kinase 2.0818871000 AB000409 MNK1 −2.0695756000 HG162-HT3165 Tyrosine Kinase Receptor Axl 2 2.0771862000 HG4243-HT4513 Zinc Finger protein Znf155 −2.0479560000 **X05299 (˜95%) major centromere autoantigen CENP-B 2.0411952000 HG2614-HT2710 Collagen Type Viii Alpha 1 2.0360297000 U02619 TFIIIC Box B-binding subunit 2.0366289000 D87937 Alpha(1,2)fucosyltransferase 5 −2.0150452000 M98045 Folylpolyglutamate synthetase −2.0156740000 *M94250 Retinoic acid inducible factor (MK) 2.0295867000 M63967 Mitochondrial aldehyde dehydrogenase x −2.0057166000 Y11306 Beta catenin/TCF-4 2.0193240000 *U60269 Putative ERVK envelope protein −2.0017337000 X59766 Zn-alpha2-glycoprotein −1.9977139000 M38258 Retinoic acid receptor gamma 1 2.0157788000 D79998 KIAA0176 −1.9967305000 U71364 Serine protase inhibitor (P19) −1.9973864000 L02867 62 kDa paraneoplastic antigen 2.0036759000 L10386 Transglutaminase E3 (TGASE3) 1.9989129000 M36429 Transducin beta-2 subunit; Also: M16538 1.9967305000 U80669 Androgen regulated homeobox protein (NKX31) −1.9772662000 HG3928-HT4198 SFTPA2D 1.9860996000 J04948 Alkaline phosphatase (ALP-1) 1.9865478000 U17969 Initiation factor eIF-5A −1.9667282000 M20681 Glucose transporter-like protein-III (GLUT3) −1.9596375000 M24594 Interferon-inducible 56 Kd protein −1.9576073000 M86826 IGF binding protein complex acid-labile subunit a 1.9715078000 M21984 (clone PWHTnT16) skeletal muscle Troponin T −1.9555675000 M35252 CO-029 −1.9542425000 *U37408 CtBP 1.9580858000 U32576 Apolipoprotein apoC-IV (APOC4) −1.9517017000 M21389 Keratin type II (58 kD) −1.9454686000 U07919 Aldehyde dehydrogenase 6 −1.9452223000 L24774 Delta3, delta2-CoA-isomerase; Also: Z25821_rna1, Z25820 1.9465301000 U37519 Aldehyde dehydrogenase (ALDH8) −1.9301847000 U12139 Alpha1(XI) collagen (COL11A1)/U12139 1.9232440000 U33920 Clone lambda 5 semaphorin 1.9253121000 S75989 Gamma-aminobutyric acid transporter type 3 −1.9180303000 V00565 Preproinsulin; Also: M10039 1.9114240000 U53442 p38Beta MAP kinase −1.9100905000 M15465 Pyruvate kinase type L; Also: D13243 −1.9063350000 K02100 Ornithine transcarbamylase (OTC) −1.8898617000 X00734 Beta-tubulin (5-beta) with ten Alu family members 1.8830934000 AB002315 KIAA0317 −1.8874766000 X04470 Antileukoprotease (ALP) from cervix uterus; Also: X04503 1.8810992000 U15932 Dual-specificity protein phosphatase −1.8727388000 X13766 Beta-casein; Also: L10615, X17070 −1.8754953000 M58297 Zinc finger protein 42 (MZF-1) −1.8720105000 D42053 KIAA0091 1.8588379000 S74445 Cellular retinoic acid-binding protein 1.8589298000 U15131 p126 (ST5) 1.8576340000 U28368 Id-related helix-loop-helix protein Id4 1.8527849000 AF006609 RGS3 1.8510028000 D49357 S-adenosylmethionine synthetase 1.8491122000 U12595 Tumor necrosis factor type 1 receptor associated protein TRAP1 −1.8570308000 U35234 Protein tyrosine phosphatase sigma 1.8379039000 S78432 Un-named-transcript-1 from SAS = transmembrane 4 protein −1.8457180000 L31881 Nuclear factor I-X 1.8350561000 U93049 SLP-76 associated protein 1.8372727000 U17743 JNK activating kinase (JNKK1); Also: L36870 −1.8407332000 Z26256 L-type calcium channel/Z26256 1.8286599000 D25539 KIAA0040 −1.8345796000 L07738 DHP-sensitive calcium channel gamma subunit (CACNLG) 1.8224950000 X06956 HALPHA44 alpha-tubulin 1.8215490000 Y10207 CD171 protein/Y10207 1.8202015000 X52056 Spi-1 proto-oncogene 1.8075350000 S81294 DCC = deleted in colorectal cancer/S81294 −1.8149132000 U28488 Putative G protein-coupled receptor (AZ3B); Also: U62027 1.8041394000 U22029 Cytochrome P450 (CYP2A7) −1.8080421000 X92896 ITBA2 protein −1.8077041000 L00137 Growth hormone releasing factor −1.8029447000 X07315 PP15 (placental protein 15) 1.7856857000 L13720 Growth-arrest-specific protein (gas) 1.7777892000 J04469 Mitochondrial creatine kinase (CKMT) −1.7906370000 U85767 Myeloid progenitor inhibitory factor-1 MPIF-1 −1.7895807000 X14830 Muscle acetylcholine receptor beta-subunit −1.7894044000 M74093 Cyclin −1.7830098000 L40407 Thyroid receptor interactor (TRIP9) 1.7708520000 X53002 Integrin beta-5 subunit; Also: J05633 1.7701153000 U87972 NAD+-isocitrate dehydrogenase/U87972 −1.7804973000 M32053 H19 RNA (spliced in silico) 1.7634280000 U27333 Alpha (1,3) fucosyltransferase (FUT6), major transcript I 1.7652959000 L40393 (clone S171) 1.7570162000 J04449 (clone NF 10) cytochrome P-450 nifedipine oxidase −1.7654823000 U03494 Transcription factor LSF −1.7667845000 U82306 Unknown protein/U82306 1.7493498000 X17094 Furin 1.7497363000 M96980 Myelin TRANSCRIPTION FACTOR 1 (MTF1) 1.7425180000 M20642 Alkali myosin light chain 1; Also: X05451, M20643 −1.7607993000 S76942 Dopamine D4 receptor; Also: L12398, HG944-HT944 −1.7606109000 U18018 E1A enhancer binding protein (E1A-F) −1.7604464000 M81933 Cdc25A 1.7403627000 HG620-HT620 Tyrosine Phosphatase Epsilon −1.7531999000 Y10506 CD110 protein/Y10506 −1.7547305000 U78524 Gu binding protein 1.7351995000 M29540 Carcinoembryonic antigen (CEA) −1.7522406000 U35113 Metastasis-associated mta1 1.7283538000 D50913 KIAA0123 −1.7435098000 M22324 Aminopeptidase N −1.7395723000 X55740 Placental cDNA coding nucleotidase (EC 3135) −1.7383841000 S81737 Alpha 1 syntrophin; Also: U40571 1.7185017000 U03399 T-complex protein 10A (TCP10A) 1.7197455000 M24351 PTH-like hormone A −1.7327287000 Y09858 Unknown protein 1.7134905000 U20428 SNC19 sequence −1.7109631000 D13633 KIAA0008 −1.7281508000 U55764 Estrogen sulfotransferase −1.7281508000 D49817 Fructose 6-phosphate 2-kinase/fructose 2 6-bisphosphatase 1.7067178000 U15197 Histo-blood group ABO protein 1.7058637000 X89109 Coronin; Also: D44497 1.7056006000 HG896-HT896 Thrombospondin 2 −1.7248900000 S70585 Thyroid-stimulating hormone alpha subunit −1.7226339000 U25433 Protein associated with tumorigenic conversion (CATR13) −1.7252989000 U82979 Ig-like transcript-3 −1.7236609000 D28383 ATP synthase B chain 1.6985355000 D29956 KIAA0055 1.6994041000 M57732 Hepatic nuclear factor 1 (TCF1) −1.7201593000 U60521 Protease proMch6 (Mch6) −1.7220166000 X52008 Strychnine binding subunit of inhibitory glycine receptor −1.7182940000 AF015950 Telomerase reverse transcriptase 1.6932872000 D78156 RasGTPase activating protein 1.6946052000 M73077 Glucocorticoid receptor repression factor 1 (GRF-1) −1.7077830000 U58681 Neurogenic basic-helix-loop-helix protein (NeuroD2) −1.7113854000 HG273-HT273 Lymphocyte Antigen Hla-G3; Also: J03027 1.6830470000 S77361 Transcript ch132/S77361 1.6826793000 M81780 SMPD1 −1.7041505000 U41804 Putative T1/ST2 receptor binding protein precursor −1.7056499000 X04706 Homeobox (clone HHO.c13); Also: X17360_rna1 −1.7052221000 U89896 Casein kinase l gamma 2 1.6789734000 HG4318-HT4588 Lim-Domain Transcription Factor Lim-1; Also: U14755 −1.6987528000 U08021 Nicotinamide N-methyltransferase (NNMT) −1.7019995000 X52228 Secreted epithelial tumor mucin antigen −1.7002709000 X73079 Encoding Polymeric Ig receptor −1.6996932000 X15331 Phosphoribosylpyrophosphate synthetase subunit one 1.6734817000 S58733 pp52 = B lymphocyte signal transduction −1.6941663000 D87077 KIAA0240 1.6707096000 U46461 Dishevelled homolog (DVL) 1.6688516000 X86018 MUF1 protein 1.6720979000 M81882 Glutamate decarboxylase (GAD65) −1.6917444000 Z38133 Myosin; Also: M36769 −1.6899744000 U83192 Post-synaptic density protein 95 (PSD95) 1.6637009000 L43579 (clone 110298)/L43579; Also: L43575 1.6584884000 U21049 DD96 1.6618127000 L24203 Ataxia-telangiectasia group D-associated protein −1.6855178000 U49248 Canalicular multispecific organic anion transporter (cMOAT) −1.6839471000 M28219 Low density lipoprotein receptor 1.6532125000 M64929 Protein phosphatase 2A alpha subunit 1.6536948000 U08096 Peripheral myelin protein-22 (PMP22) non-coding 1B/U08096 1.6565773000 M27749 Ig-related 14.1 protein −1.6814674000 S38742 HOX11 = HOX11 homeodomain {homeobox}; Also: M75952 −1.6780629000 U45983 G protein-coupled receptor GPR-CY6 −1.6801088000 X95240 Cysteine-rich secretory protein-3; Also: X94323 −1.6780629000 J02854 20-kDa myosin light chain (MLC-2) −1.6748611000 D38081 Thromboxane A2 receptor 1.6459133000 D82346 HNSPC 1.6449307000 D88799 Cadherin 1.6468936000 M59820 Granulocyte colony-stimulating factor receptor (CSF3R) 1.6444386000 U33838 NF-kappa-B p65delta3, spliced transcript −1.6690843000 AF002224 E6-AP ubiquitin protein ligase 3A/promoter P1 1.6389882000 X16260 Inter-alpha-trypsin inhibitor subunit 3; Also: X69532_rna1 1.6379898000 D21063 KIAA0030 −1.6641717000 Z19574 Cytokeratin 17 −1.6662839000 U68723 Checkpoint suppressor 1 1.6359861000 D90064 CGM6 CD66b (NCA-95) −1.6611025000 U05012 Receptor tyrosine kinase TrkC (NTRK3); Also: S76475 −1.6618127000 M14219 Chondroitin/dermatan sulfate proteoglycan (PG40) core protein 1.6324573000 X97444 Transmembrane protein Tmp21-llex/X97444 1.6294096000 Z11502 Intestine-specific annexin 1.6304279000 M84526 Adipsin/complement factor D 1.6235563000 U81523 Endometrial bleeding associated factor 1.6268534000 X87212 Cathepsin C 1.6242821000 D29640 KIAA0051; Also: L33075 −1.6490914000 U32674 Orphan receptor GPR9 (GPR9); Also: X95876 −1.6466487000 X65873 Kinesin (heavy chain) 1.6154240000 X70218 Protein phosphatase X 1.6133132000 M59371 Protein tyrosine kinase −1.6414741000 U43916 Tumor-associated membrane protein homolog (TMP) −1.6337209000 U33429 K+ channel beta 2 subunit 1.6047659000 X16706 Fra-2 1.6036815000 X90780 Cardiac troponin I 1.6063814000 X76498 Uterine bombesin receptor −1.6276219000 HG3893-HT4163 Phosphoglucomutase 1 1.6009729000 S83308 SOX5 = Sry-related HMG box 1.6009729000 U64197 Chemokine exodus 1.5982432000 K02777 T-cell receptor active alpha-chain from Jurkat cell line −1.6260836000 U07794 Tyrosine kinase (TXK) −1.6227320000 X98337 Complement factor H-related protein 4; Also: X68679 −1.6271097000 D29992 Placental protein 5 (PP5) 1.5932861000 X51698 Spasmolytic polypeptide (SP); Also: U47292 1.5971465000 AF005887 ATF family member ATF6 −1.6211763000 HG3432-HT3618 Fibroblast Growth Factor Receptor K-Sam −1.6198756000 HG537-HT537 Collagen Type Viii Alpha 2 −1.6188323000 M60278 Heparin-binding EGF-like growth factor −1.6216955000 M83738 Protein-tyrosine phosphatase (PTPase MEG2) −1.6175245000 X99975 hRTR/hGCNF protein −1.6188323000 U40223 Uridine nucleotide receptor (UNR) 1.5888317000 M84820 Retinoid X receptor beta (RXR-beta); Also: X63522, X65463 −1.6172546000 U04313 Maspin −1.6143698000 U16997 Orphan receptor ROR gamma −1.6173935000

[0031] TABLE 7 Gene targets in MS spinal cord white matter from a sample with inflammation by macrophages and demyelination. Probe set Gene description log10 (ratio) fold chang *M63438 Ig rearranged gamma chain, V-J-C region 3.0608377000 HG1614-HT1614 Protein Phosphatase 1 Alpha Catalytic Subunit −2.6832272000 L76200 Guanylate kinase (GUK1) −2.6705781000 U02619 TFIIIC Box B-binding subunit 2.7524326000 M91083 DNA-binding protein (HRC1) 2.7402837000 U35234 Protein tyrosine phosphatase sigma 2.7303381000 M95787 22 kDa smooth muscle protein (SM22) −2.6407546000 M13755 Interferon-induced 17-kDa/15-kDa protein −2.6319001000 U72507 40871 sequence −2.5803547000 *M87789 Anti-hepatitis A IgG V, C, CDR regions 2.5829467000 L41143 Pseudo TCTA at t(1; 3) translocation site 2.5372864000 S68616 Na+/H+ exchanger NHE-1 isom −2.5223464000 X00734 Beta-tubulin (5-beta) with ten Alu family members 2.4960990000 J04948 Alkaline phosphatase (ALP-1) 2.4679779000 AB002318 KIAA0320 −2.4959950000 M27826 Endogenous retroviral protease −2.4913967000 X79882 Irp −2.4741434000 S73885 AP-4 = basic helix-loop-helix DNA-binding protein −2.4527445000 U12707 Wiskott-Aldrich syndrome protein (WASP) 2.4106085000 X12517 U1 small nuclear RNP-specific C protein 2.4070508000 D84361 p52 and p64 N-Shc −2.4451759000 M21388 Unproductively rearranged Ig mu-chain V-region VD −2.4238600000 D87452 KIAA0263 −2.4207394000 U12139 Alpha1(XI) collagen (COL11A1)/U12139 2.3716219000 U45328 Ubiquitin-conjugating enzyme (UBE2I) 2.3701682000 *U37408 CtBP 2.3659557000 D26561 ORF E7 from papillomavirus 5b genome −2.4064124000 U40490 Nicotinamide nucleotide transhydrogenase 2.3468418000 M60299 Alpha-1 collagen type II s 1 2 and 3/M60299 2.3402458000 U22970 16-Jun (interferon-inducible peptide precursor) −2.3853381000 AF002224 E6-AP ubiquitin protein ligase 3A/promoter P1 2.3358589000 L77213 Phosphomevalonate kinase −2.3777159000 U40223 Uridine nucleotide receptor (UNR) 2.3265407000 HG162-HT3165 Tyrosine Kinase Receptor Axl 2 2.3128118000 J02947 Extracellular-superoxide dismutase (SOD3) 2.3059959000 AF015910 Unknown protein −2.3407910000 L08246 Myeloid cell differentiation protein (MCL1) −2.3375591000 D87433 KIAA0246 −2.3191061000 U86759 Netrin-2 like protein (NTN2I); Also: U86758_rna1 2.2712606000 X07315 PP15 (placental prot 15) 2.2678754000 D86977 KIAA0224 −2.3159179000 M22632 Mitochondrial aspartate aminotransferase −2.3137091000 X71135 Sox3 2.2587570000 AB000895 Cadherin FIB1 −2.3095154000 Z26256 L-type calcium channel/Z26256 2.2564772000 D42053 KIAA0091 2.2499318000 *D61391 Phosphoribosypyrophosphate synthetase-associated protein 39 −2.2951821000 M58286 TNF receptor; Also: M63121, M33294, X55313, M75866 −2.2938596000 U02566 Receptor tyrosine kinase tif; Also: U18934 −2.2947417000 U60116 Skeletal muscle LIM-prot SLIM2 2.2412974000 X89416 Protein phosphatase 5 2.2405866000 D90084 Pyruvate dehydrogenase alpha subunit −2.2917018000 M16653 Pancreatic elastase IIB −2.2924222000 D25303 Integrin alpha subunit −2.2749656000 X81420 hHKb1 protein 2.2188077000 AD000092 RAD23A homolog −2.2698630000 L19711 Dystroglycan (DAG1) −2.2611439000 D31833 Vasopressin V1b receptor; Also: L37112 2.2053397000 J05582 Pancreatic mucin; Also: J05581 2.2060018000 L24774 Delta3, delta2-CoA-isomerase; Also: Z25821_rna1, Z25820 2.2038512000 M84739 Autoantigen calreticulin 2.2049335000 U37219 Cyclophilin-like protein CyP-60 −2.2546151000 L38517 Indian hedgehog protein (IHH) 2.1964718000 U51010 Nicotinamide N-methyltransferase 1 and 5 ing region 2.1883659000 M24400 Chymotrypsinogen 2.1859669000 U05861 Hepatic dihydrodiol dehydrogenase −2.2392995000 X67325 p27 −2.2399248000 U23803 Heterogeneous ribonucleoprotein A0 2.1817007000 X54637 Tyk2 non-receptor protein tyrosine kinase 2.1769590000 D15049 Protein tyrosine phosphatase −2.2322971000 *X64072 CD18; Also: M15395 2.1707017000 AF000545 Putative purinergic receptor P2Y10 −2.2244036000 D50855 Ca-sensing receptor; Also: U20760, U20759 −2.2251800000 U37221 Cyclophilin-like protein 2.1582117000 L02321 Glutathione S-transferase (GSTM5) −2.2208922000 K03189 Chorionic gonadotropin beta subunit 2.1563977000 M34344 Platelet glycoprotein IIb (GPIIb) −2.2134513000 X04201 Skeletal muscle tropomyosin −2.2087772000 *M85220 Heavy chain disease IgA chain CH3 region 2.1465908000 X59842 PBX2; Also: U89336_2, D28769_1, X80700_rna1 2.1397217000 Z49254 L23-related −2.2020794000 M21665 Beta-myosin heavy chain; Also: X52889 2.1256439000 M94167 Heregulin-beta2 2.1230345000 X52896 Dermal fibroblast elastin; Also: HG2994-HT4851 2.1256439000 D38305 Tob −2.1898507000 U66559 Anaplastic lymphoma kinase receptor −2.1918002000 D13635 KIAA0010 2.1218880000 M34376 Beta-microseminoprotein (MSP); Also: X57928 2.1207384000 X14767 GABA-A receptor, beta 1 subunit −2.1846914000 X17651 Myf-4 myogenic determination factor −2.1869563000 L38929 Protein tyrosine phosphatase delta 2.1154441000 M25809 Endomembrane proton pump subunit 2.1134085000 HG3570-HT3773 Protein Phosphatase Inhibitor Homolog −2.1780412000 M92287 Cyclin D3 (CCND3) −2.1800542000 M77698 GLI-Krupple related protein (YY1) −2.1748590000 D43767 Chemokine −2.1684238000 *U52518 Grb2-related adaptor protein (Grap) 2.0925452000 U27333 Alpha (1,3) fucosyltransferase (FUT6), major transcript I 2.0845763000 J05252 Also: M95971 2.0731683000 U23430 Cholecystokinin type A receptor (CCK-A); Also: L19315 2.0766404000 HG3934-HT4204 G1 Phase-Specific −2.1499116000 X99142 Hair keratin hHb6 2.0715138000 L00205 K6b epidermal keratin type II −2.1467480000 M35128 Muscarinic acetylcholine receptor −2.1447706000 S85963 hIRS-1 = rat insulin receptor substrate-1 homolog 2.0629578000 X63359 UGT2BIO udp glucuronosyltransferase 2.0668847000 HG4518-HT4921 Transcription Factor Btf3 Homolog M90355 2.0608866000 M25269 Tyrosine kinase (ELK1) onco 2.0620176000 HG2755-HT2862 T-Plastin −2.1371958000 L25878 p33/HEH epoxide hydrolase (EPHX) −2.1326599000 X95406 Cyclin E −2.1339379000 D80003 KIAA0181 −2.1313780000 M80563 CAPL protein −2.1310570000 *U28811 Cysteine-rich fibroblast growth factor receptor (CFR-1) −2.1317790000 HG4068-HT4338 Phosphoprotein Tal2 2.0472749000 S80335 Integrin beta 7 subunit 2.0451273000 D14822 CBFA2T1 −2.1245042000 J02783 Thyroid hormone binding protein (p55) −2.1270238000 M36089 DNA-repair protein (XRCC1) 2.0374878000 U42412 AMP-activated protein kinase gamma-1 subunit −2.1207384000 X12433 pHS1-2 with ORF homolog to membrane receptor proteins −2.1131910000 D88799 Cadherin 2.0236639000 X15331 Phosphoribosylpyrophosphate synthetase subunit one 2.0203613000 U65011 Preferentially expressed antigen of melanoma (PRAME) −2.1092410000 D30755 KIAA0113 −2.1044871000 D50930 KIAA0140 −2.1026052000 U20428 SNC19 sequence 2.0117818000 U83192 Post-synaptic density protein 95 (PSD95) 2.0096633000 HG2825-HT2949 Ret Transforming −2.0982045000 M28825 Thymocyte antigen CD1a −2.0982975000 AC002086 PAC clone DJ525N14/Xq23 2.0030295000 L02867 62 kDa paraneoplastic antigen 2.0034605000 ***D16480 Mitochondrial enoylCoA hydratase 1.9986952000 U65404 Erythroid-specific TRANSCRIPTION FACTOR EKLF 2.0002171000 L10386 Transglutaminase E3 (TGASE3) 1.9951963000 L05500 Fetal brain adenylyl cyclase 1.9921115000 U15655 Ets domain prot ERF 1.9914476000 M16405 m4 muscarinic acetylcholine receptor −2.0841292000 X86570 Acidic hair keratin 1 −2.0854690000 D82345 NB thymosin beta 1.9813655000 U15131 p126 (ST5) 1.9820450000 U17838 Zinc finger protein RIZ −2.0785474000 M75106 Prepro-plasma carboxypeptidase B 1.9738203000 D12625 Neurofibromin 1.9633155000 U83843 HIV-1 Nef interacting prot (Nip7-1)/U83843 1.9644953000 U96769 Chondroadherin 1.9654369000 Z48512 XG (clone PEP6)/Z48512 −2.0719740000 D87078 KIAA0235 1.9580858000 M36429 Transducin beta-2 subunit; Also: M16538 1.9609462000 M58026 NB-1 1.9609462000 U33920 Clone lambda 5 semaphorin 1.9607086000 D83920 Uterus ficolin-1 1.9572406000 X80910 PPP1CB −2.0673499000 AB000897 Cadherin FIB3 −2.0600365000 M86933 Amelogenin (AMELY); Also: M55419, U79549_rna1, M55418 −2.0580462000 X79066 ERF-1 −2.0611559000 X60486 H4/g H4 histone −2.0529824000 D28532 Renal Na+-dependent phosphate cotransporter −2.0486360000 L41668 UDP Galactose 4 epimerase −2.0491211000 U16031 TRANSCRIPTION FACTOR IL-4 Stat −2.0447357000 U84540 Dystrobrevin isom DTN-3 (DTN)/U84540 −2.0471775000 X01715 Acetylcholine receptor gamma subunit precursor −2.0451273000 HG3033-HT3194 Spliceosomal protein Sap 62 1.9207327000 L41066 NF-AT3 1.9175055000 U57057 WD protein IR10 1.9214263000 AF001294 IPL −2.0404143000 M60614 Wilms tumor (WIT-1) associated protein −2.0378248000 HG2417-HT2513 Dynein Heavy Chain 1.9066044000 M61199 Cleavage signal 1 protein 1.9057959000 J04611 Lupus p70 (Ku) autoantigen protein −2.0357298000 L38503 Glutathione S-transferase theta 2 (GSTT2) −2.0343276000 X17098 PSG10 pregnancy specific glycoprotein 10 1.9014583000 X74328 CB2 (peripheral) cannabinoid receptor 1.8987252000 D82060 Kidney histidine rich putative membrane protein −2.0292823000 J04056 Carbonyl reductase −2.0295867000 M23263 Androgen receptor −2.0285713000 HG3945-HT4215 Phospholipid Transfer protein 1.8887410000 M23294 Beta-hexosaminidase beta-subunit (HEXB) 1.8878985000 M96684 Pur (pur-alpha) 1.8895818000 L17327 Pre-T/NK cell associated protein (3B3) −2.0245883000 M19888 Small proline rich protein (sprl), clone 128 −2.0258177000 S79873 H-lamp-2 = lysosome-associated membrane protein-2 −2.0271457000 X57351 1-8D from interferon-inducible family −2.0254083000 X74819 Cardiac troponin T 1.8825245000 M55621 N-acetylglucosaminyltransferase I (GlcNAc-TI) 1.8793826000 Z36714 Cyclin F 1.8788089000 D84239 lgG Fc binding protein −2.0175732000 S72370 Pyruvate carboxylase −2.0198430000 U24576 Breast tumor autoantigen sequence −2.0212927000 HG172-HT3924 Spermidine/Spermine N1-Acetyltransferase 1.8767950000 X63755 High-sulphur keratin 1.8709888000 D87937 Alpha(1,2)fucosyltransferase 5 −2.0150452000 M62324 Modulator recognition factor I (MRF-1) −2.0143105000 U22377 Zn-15 related zinc finger protein (rlf) 1.8588379000 D28588 KIAA0048 −2.0045363000 M63967 Mitochondrial aldehyde dehydrogenase x −2.0057166000 X02176 Complement component C9; Also: K02766 1.8488047000 D86983 KIAA0230 1.8450337000 D49818 Fructose 6-phosphate 2-kinase/fructose 2 6-bisphosphatase 1.8366405000 L29218 Clk2 1.8374843000 U09002 NMDA receptor modulatory subunit 2A (hNR2A) 1.8334659000 HG4683-HT5108 Tumor Necrosis Factor Receptor 2 Associated protein Trap3 −1.9940971000 L13391 Helix-loop-helix basic phosphoprotein (G0S8) −1.9964022000 M98447 Keratinocyte transglutaminase −1.9956352000 U71364 Serine protase inhibitor (P19) −1.9973864000 X63629 P cadherin −1.9925535000 X80695 OXA1Hs −1.9965117000 X98482 TNNT2 11/X98482 1.8299467000 X59618 RR2 small subunit ribonucleotide reductase 1.8267225000 X93996 AFX protein 1.8234742000 D29992 Placental protein 5 (PP5) 1.8175654000 J04970 Carboxypeptidase M 1.8224950000 X04729 Plasminogen activator inhibitor type 1 N-terminus/X04729 1.8175654000 D31797 CD40 ligand −1.9855387000 HG3578-HT3781 Autoimmune Antigen Thyroid Disease-Related Antigen 1.8123589000 *M13241 N-myc 1.8081145000 U05875 Interferon gamma receptor accessory factor-1 (AF-1) 1.8044061000 X04500 Prointerleukin 1 beta 1.8068580000 X92106 Bleomycin hydrolase 1.8020893000 U21049 DD96 1.7944880000 U91931 AP-3 complex beta3A subunit 1.7944880000 HG4593-HT4998 Sodium Channel 1 −1.9746268000 M15881 Uromodulin (Tamm-Horsfall glycoprotein) −1.9748570000 D80004 KIAA0182 −1.9684829000 M13699 Ceruloplasmin (ferroxidase) 1.7788745000 D87449 KIAA0260 1.7770642000 M36803 Hemopexin 1.7759743000 S62028 Recoverin; Also: S43855 1.7756104000 X06182 C-kit proto-oncogene; Also: HG2549-HT3951 1.7745170000 M55682 Cartilage matrix protein (CMP); Also: M55683 1.7715875000 U17077 BENE 1.7678976000 HG3921-HT4191 Homeotic protein C6, Class I −1.9577270000 M20681 Glucose transporter-like protein-III (GLUT3) −1.9596375000 U78180 Sodium channel 2 (hBNaC2) −1.9604708000 D88795 Cadherin −1.9559282000 L34587 RNA polymerase II elongation factor SIII p15 subunit −1.9548453000 M21984 (clone PWHTnT16) skeletal muscle Troponin T −1.9555675000 U37248 Alpha-mannosidase (6A8) −1.9553269000 U45285 Specific 116-kDa vacuolar proton pump subunit (OC-116 KDa) −1.9530345000 Z29083 5T4 Oncofetal antigen −1.9550862000 X99140 Hair keratin hHb5 1.7489629000

[0032] TABLE 8 Gene targets in MS spinal cord white matter from a sample with inflammation by macrophages and lymphocytes and demyelination. Probe set Gene description log10 (ratio) fold change *M63438 Ig rearranged gamma chain, V-J-C region; Also: X96754 3.5479855000 L76200 Guanylate kinase (GUK1) −2.6727442000 *M87789 Anti-hepatitis A IgG V, C, CDR regions; Also: J00221_2 2.9066259000 X74570 Gal-beta(1-3/1-4)GlcNAc alpha-23-sialyltransferase −2.5341531000 HG3033-HT3194 Spliceosomal protein Sap 62 2.6505720000 HG3945-HT4215 Phospholipid Transfer protein 2.6058005000 D84361 p52 and p64 N-Shc −2.4451759000 D50402 NRAMP1 2.4524994000 D26561 ORF E7 from papillomavirus 5b genome −2.4064124000 U22970 16-Jun (interferon-inducible peptide precursor); Also: U22970 −2.3853381000 L27080 Melanocortin 5 receptor (MC5R) 2.3691787000 M84739 Autoantigen calreticulin 2.3240457000 D49817 Fructose 6-phosphate 2-kinase/fructose 2 6-bisphosphatase 2.3082442000 M96326 Azurocidin −2.3481101000 HG3286-HT3463 Crystallin Alpha A −2.3455208000 J03600 Lipoxygenase −2.3282267000 L32976 Protein kinase (MLK-3) −2.3323880000 M80397 DNA polymerase delta catalytic subunit; Also: M81735 −2.3273589000 J04948 Alkaline phosphatase (ALP-1) 2.2624986000 AB000895 Cadherin FIB1 −2.3181155000 Y00757 Polypeptide 7B2 −2.3219607000 X99142 Hair keratin hHb6 2.2411728000 *D61391 Phosphoribosypyrophosphate synthase-associated protein39 −2.2951821000 Y08409 Spot14 −2.2876898000 L14565 Peripherin (PRPH) s 1-9 2.2002210000 D13988 Rab GDI 2.1970461000 M23294 Beta-hexosaminidase beta-subunit (HEXB) 2.1922189000 U15131 p126 (ST5) 2.1918421000 HG2614-HT2710 Collagen Type Viii Alpha 1 2.1829707000 U37219 Cyclophilin-like protein CyP-60 −2.2589364000 U56816 Kinase Myt1 (Myt1) −2.2537014000 U45328 Ubiquitin-conjugating enzyme (UBE2I); Also: U31882 2.1722622000 X67325 p27 −2.2399248000 *M94250 Retinoic acid inducible factor (MK) 2.1555486000 M55621 N-acetylglucosaminyltransferase I (GlcNAc-TI) 2.1510939000 J02947 Extracellular-superoxide dismutase (SOD3); Also: U10116 2.1296738000 U35234 Protein tyrosine phosphatase sigma 2.1262938000 X53683 LAG-1 −2.1972116000 X17651 Myf-4 myogenic determination factor −2.1869563000 HG3570-HT3773 Protein Phosphatase Inhibitor Homolog −2.1780412000 D10495 Protein kinase C delta-type 2.0939642000 M38258 Retinoic acid receptor gamma 1 2.0938243000 M27161 MHC class I CD8 alpha-chain (Leu-2/T8) −2.1755118000 U13706 ELAV-like neuronal protein 1 isom Hel-N2 (Hel-N1)/U13706 −2.1692335000 X15331 Phosphoribosylpyrophosphate synthetase subunit one 2.0852549000 U87964 Putative G-protein (GP-1) −2.1662080000 U77643 K12 protein precursor 2.0813599000 HG3987-HT4257 Cpg-Enriched Dna Clone E06 −2.1621161000 U12707 Wiskott-Aldrich syndrome protein (WASP); Also: U19927 2.0746519000 AB000462 SH3 binding RES4-23A −2.1517587000 U12139 Alpha1(XI) collagen (COL11A1)/U12139 2.0644580000 X54637 Tyk2 non-receptor protein tyrosine kinase 2.0618105000 D49490 Disulfide isomerase-related protein −2.1380657000 X95406 Cyclin E −2.1339379000 M63582 Preprothyrotropin-releasing hormone −2.1266184000 D14827 Tax helper protein 1 −2.1194209000 L29433 Factor X (blood coagulation factor) 2.0325785000 U93049 SLP-76 associated protein 2.0340667000 D83784 KIAA0198 −2.1156937000 D63486 KIAA0152 2.0280830000 L16991 Thymidylate kinase (CDC8) 2.0283882000 U15197 Histo-blood group ABO protein 2.0293026000 HG3242-HT4231 Calcium Channel, Voltage-Gated, Alpha 1e Subunit, 3 −2.1080574000 U65011 Preferentially expressed antigen of melanoma (PRAME) −2.1092410000 U82310 Unknown protein/U82310 −2.1044871000 HG2290-HT2386 Calcitonin −2.1007151000 M28825 Thymocyte antigen CD1a −2.0982975000 X57110 HG642-HT642 and others −2.0995943000 M31776 M25296 and others 2.0134061000 Y08263 AAD14 protein −2.0928083000 U77968 Neuronal PAS1 (NPAS1) 2.0047512000 L38487 Estrogen receptor-related protein (hERRa1) −2.0839503000 M16405 m4 muscarinic acetylcholine receptor −2.0841292000 U96769 Chondroadherin 1.9994350000 U83192 Post-synaptic density protein 95 (PSD95) 1.9963584000 X79066 ERF-1 −2.0739931000 AB000409 MNK1 −2.0695756000 Z48512 XG (clone PEP6)/Z48512 −2.0719740000 X60486 H4/g H4 histone −2.0529824000 L24774 Delta3, delta2-CoA-isomerase; Also: Z25821_rna1, Z25820 1.9747715000 U79273 Clone 23933 sequence 1.9728737000 X04898 Apolipoprotein AII 1.9733099000 X07315 PP15 (placental protein 15) 1.9728968000 L41668 UDP Galactose 4 epimerase −2.0491211000 AF008445 Phospholipid scramblase 1.9705328000 AF001294 IPL −2.0447357000 D13636 KIAA0011 −2.0416887000 L08488 Inositol polyphosphate 1-phosphatase 1.9596625000 Z48314 Apomucin; Also: U06711 1.9617769000 J04056 Carbonyl reductase −2.0295867000 M21904 4F2 glycosylated heavy chain (4F2HC) antigen 1.9515075000 *X64072 CD18; Also: M15395 1.9479481000 U23430 Cholecystokinin type A receptor (CCK-A); Also: L19315 1.9457393000 M62324 Modulator recognition factor I (MRF-1) −2.0143105000 D21851 KIAA0028 −2.0075344000 X64037 RNA polymerase II associated protein RAP74 −2.0115704000 U83303 GCP-2 (granulocyte chemotactic protein-2) −2.0065730000 HG162-HT3165 Tyrosine Kinase Receptor Axl 2 1.9327020000 M81933 Cdc25A 1.9346247000 X04500 Prointerleukin 1 beta 1.9345489000 M61199 Cleavage signal 1 protein 1.9318391000 U28831 Protein immuno-reactive with anti-PTH polyclonal antibodies 1.9287542000 U35113 Metastasis-associated mta1 1.9319915000 X92106 Bleomycin hydrolase 1.9279859000 D79998 KIAA0176 −1.9967305000 HG4683-HT5108 Tumor Necrosis Factor Receptor 2 Associated protein Trap3 −1.9940971000 U71364 Serine protase inhibitor (P19) −1.9973864000 U78524 Gu binding protein 1.9260336000 X17098 PSG10 pregnancy specific glycoprotein 10 1.9229848000 M15881 Uromodulin (Tamm-Horsfall glycoprotein) −1.9748570000 D42053 KIAA0091 1.9100104000 M19311 Calmodulin 1.9089673000 HG3921-HT4191 Homeotic protein C6, Class I −1.9577270000 U78180 Sodium channel 2 (hBNaC2) −1.9604708000 L41143 Expressed pseudo TCTA at t(1; 3) translocation site 1.8975177000 M21984 (clone PWHTnT16) skeletal muscle Troponin T −1.9555675000 Z29083 5T4 Oncofetal antigen −1.9550862000 L36463 Ras inhibitor (Rin1) 1.8962506000 U32576 Apolipoprotein apoC-IV (APOC4) −1.9517017000 X13839 Vascular smooth muscle alpha-actin −1.9479070000 L35240 Enigma −1.9442358000 X07695 Cytokeratin 4 −1.9460836000 X89101 Fas (Apo-1, CD95)./X89101; Also: X83493, X63717, X83492 −1.9459607000 U15655 Ets domain protein ERF 1.8889934000 U02082 Guanine nucleotide regulatory protein (tim1) −1.9407654000 U11690 Faciogenital dysplasia (FGD1) 1.8867726000 U65404 Erythroid-specific TRANSCRIPTION FACTORS EKLF 1.8825245000 U82818 UCP3S/U82818 1.8860826000 M96980 Myelin TRANSCRIPTION FACTORS 1 (MTF1) 1.8786190000 X93996 AFX protein 1.8819835000 D10511 Mitochondrial acetoacetyl-CoA thiolase −1.9274987000 D79985 KIAA0163 −1.9194703000 M84424 Cathepsin E (CTSE) −1.9196010000 M36089 DNA-repair protein (XRCC1) 1.8706560000 U02619 TFIIIC Box B-binding subunit 1.8707549000 U17566 65 kDa hydrophobic protein 1.8723894000 *L05624 MAP kinase kinase; Also: L11284 1.8667598000 U28488 Putative G protein-coupled receptor (AZ3B); Also: U62027 1.8656961000 J03171 Interferon-alpha receptor (HuIFN-alpha-Rec) −1.9122221000 U53442 p38Beta MAP kinase −1.9100905000 M15465 Pyruvate kinase type L; Also: D13243 −1.9063350000 X87870 Hepatocyte nuclear factor 4a −1.9037680000 HG4390-HT4660 Ribosomal protein L18a Homolog 1.8601583000 *U37408 CtBP 1.8621016000 Z78289 (clone 1D2)/Z78289 1.8617404000 M11722 Terminal transferase 1.8534244000 HG831-HT831 Potassium Channel −1.8930679000 J00220 IGHA1 from Ig germline H-chain G-E-A region A: gamma-3 5 1.8475357000 M59820 Granulocyte colony-stimulating factor receptor (CSF3R) 1.8484047000 K02100 Ornithine transcarbamylase (OTC) −1.8898617000 L21998 Intestinal mucin (MUC2) −1.8902813000 U06698 Neuronal kinesin heavy chain −1.8904210000 U68233 Farnesol receptor HRR-1 (HRR-1) −1.8884603000 M34516 Omega light chain protein 14.1 (Ig lambda chain related) 1.8469395000 M36429 Transducin beta-2 subunit; Also: M16538 1.8443529000 U29615 Chitotriosidase precursor 1.8448808000 U60116 Skeletal muscle LIM-protein SLIM2 1.8436687000 X60655 EVX1 1.8447256000 M74525 HHR6B (yeast RAD 6 homolog) −1.8828090000 Z71389 Skin-antimicrobial-peptide 1 (SAP1)/Z71389 −1.8800987000 U15932 Dual-specificity protein phosphatase −1.8727388000 X13766 Beta-casein; Also: L10615, X17070 −1.8754953000 D82346 HNSPC 1.8354052000 AF009674 Axin −1.8701112000 U65093 Msg1-related 1 (mrg1) −1.8704039000 U67733 Cyclic nucleotide phosphodiesterase PDE2A3 1.8279505000 *X13334 CD14 myeloid cell-specific leucine-rich glycoprotein 1.8282409000 AF000231 Rab11a GTPase −1.8662873000 D83782 KIAA0199 −1.8634716000 Z29331 (23 k/3) ubiquitin-conjugating enzyme UbcH2 1.8257506000 Y10262 EYA3/Y10262; Also: U81602 −1.8571817000 L47276 (cell line HL-60) alpha topoisomerase/L47276; Also: L47277 −1.8492658000 M57567 ADP-ribosylation factor (hARF5) −1.8489585000 U51587 Golgi complex autoantigen golgin-97 −1.8501866000 U59058 Beta-A3/A1 crystallin (CYRBA3/A1); Also: M14306 −1.8490726000 HG909-HT909 Mg81 1.8123176000 U17743 JNK activating kinase (JNKK1); Also: L36870 −1.8407332000 J05582 Pancreatic mucin; Also: J05581 1.8041208000 Z35309 Adenylyl cyclase −1.8325089000 L13720 Growth-arrest-specific protein (gas) 1.8010262000 U83843 HIV-1 Nef interacting protein (Nip7-1)/U83843 1.7976829000 X70683 SOX-4 protein 1.7998573000 M60746 Histone H3.1 (H1F3) −1.8265607000 U27333 Alpha (1,3) fucosyltransferase (FUT6), major transcript I 1.7928468000 U33920 Clone lambda 5 semaphorin 1.7951150000 Z69881 Adenosine triphosphatase calcium −1.8223316000 U08096 Peripheral myelin protein-22 (PMP22) 1B/U08096 1.7898979000 U48861 Beta 4 nicotinic acetylcholine receptor subunit 1.7900387000 S81294 DCC = deleted in colorectal cancer/S81294 −1.8149132000 L01406 Growth hormone-releasing hormone receptor 1.7840464000 M91585 Br140 1.7844746000 D11094 MSS1 1.7794161000 L31881 Nuclear factor I-X 1.7732377000 M24486 Prolyl 4-hydroxylase alpha subunit; Also: M24487, U14620_1 1.7737864000 HG4115-HT4385 Olfactory Receptor Or17-210 −1.7984780000 L38929 Protein tyrosine phosphatase delta 1.7706311000 U43843 H-neuro-d4 prot −1.7955324000 M13981 Inhibin A-subunit 1.7638022000 M25269 Tyrosine kinase (ELK1) 1.7632033000 U67611 Mouse transaldolase/U67611 1.7644277000 Z26256 L-type calcium channel/Z26256 1.7674898000 X14830 Muscle acetylcholine receptor beta-subunit −1.7894044000 L22548 Collagen type XVIII alpha 1 (COL18A1) 1.7594412000 X53296 IRAP; Also: X64532_rna1, X52015 1.7616648000 X81420 hHKb1 prot 1.7594729000 D49818 Fructose 6-phosphate 2-kinase/fructose 2 6-bisphosphatase 1.7560272000 HG3884-HT4154 Homeotic protein Hpx-42 1.7532382000 M64929 Protein phosphatase 2A alpha subunit 1.7537745000 U06088 N-acetylgalactosamine 6-sulphatase (GALNS) −1.7779703000 U77846 Elastin −1.7806773000 U87972 NAD+-isocitrate dehydrogenase/U87972 −1.7804973000 D49357 S-adenosylmethionine synthetase 1.7486144000 X86401 L-arginine: glycine amidinotransferase; Also: S68805 1.7521582000 X07876 Irp protein (int-1 related protein) −1.7772455000 X52011 MYF6 encoding a muscle determination factor −1.7734207000 *M24766 Alpha-2 collagen type IV (COL4A2); Also: X05610 1.7465174000 M58026 NB-1 1.7429214000 U22377 Zn-15 related zinc finger protein (rlf) 1.7474118000 U28368 Id-related helix-loop-helix protein Id4 1.7455432000 X13293 B-myb 1.7445668000 X53002 Integrin beta-5 subunit; Also: J05633 1.7436665000 L41919 HIC-1 fragment −1.7691926000 M11186 Prepro-oxytocin-neurophysin I (OXT) −1.7693773000 M96684 Pur (pur-alpha) 1.7398096000 X65873 Kinesin (heavy chain) 1.7411122000 J04449 (clone NF 10) cytochrome P-450 nifedipine oxidase −1.7654823000 U28131 HMGI-C chimeric transcript −1.7626786000 X87160 Epithelial amiloride-sensitive sodium channel gamma 1.7337989000 M20642 Alkali myosin light chain 1; Also: X05451, M20643 −1.7607993000 U59111 Dermatan sulfate proteoglycan 3 (DSPG3) −1.7585334000 M77829 Channel-like integral membrane protein (CHIP28) 1.7323536000 X16260 Inter-alpha-trypsin inhibitor subunit 3; Also: X69532_rna1 1.7297721000 X68090 Fc-gamma-RIIA IgG Fc receptor class IIA/X68090 1.7286378000 X68836 S-adenosylmethionine synthetase 1.7323133000 HG620-HT620 Tyrosine Phosphatase Epsilon −1.7531999000 L43964 (clone F-T03796) STM-2 −1.7531999000 X96753 Chondroitin sulfate proteoglycan (MCSP) −1.7562556000 Y10506 CD110 protein/Y10506 −1.7547305000 M91083 DNA-binding protein (HRC1) 1.7237839000 L34155 Laminin-related protein (LamA3) −1.7485756000 X66362 PCTAIRE-3 serine/threonine protein kinase −1.7478001000 AF005361 Importin alpha 6 −1.7435098000 D50913 KIAA0123 −1.7435098000 M91196 DNA-binding protein (HRC1) −1.7448795000 X17094 Furin 1.7140782000 X56199 XIST a (locus DXS399E) 1.7144136000 X90872 gp25L2 protein 1.7174239000 M22324 Aminopeptidase N −1.7395723000 *M74826 Glutamate decarboxylase (GAD-2) −1.7407573000 U71203 Rit; Also: Y07566 −1.7377888000 X63359 UGT2BIO udp glucuronosyltransferase 1.7031624000 X97444 Transmembrane protein Tmp21-liex./X97444 1.7065898000

[0033] TABLE 9 Gene targets in MS spinal cord white matter from a sample with axonal loss. Probe set Gene description log10 (ratio) fold change *M63438 Ig rearranged gamma chain, V-J-C region; Also: X96754 3.9579713000 AB000584 TGF-beta superfamily protein −2.9495730000 *M87789 Anti-hepatitis A IgG V, C, CDR regions; J00221 3.3816210000 L76200 Guanylate kinase (GUK1) −2.6727442000 M27504 Topoisomerase type II (Topo II)/M27504/Also: Z15115 3.0841507000 M84739 Autoantigen calreticulin 2.9484496000 U45878 Inhibitor of apoptosis protein 1; Also: L49432 −2.5991459000 U22398 Cdk-inhibitor p57KIP2 (KIP2) −2.5926486000 HG3033-HT3194 Spliceosomal protein Sap 62 2.7255114000 J04794 Aldehyde reductase −2.5857708000 M24486 Prolyl 4-hydroxylase alpha subunit; Also: M24487, U14620_1 2.4710569000 X74570 Gal-beta(1-3/1-4)GlcNAc alpha-23-sialyltransferase −2.5341531000 D64142 Histone H1x −2.5299434000 M21904 4F2 glycosylated heavy chain (4F2HC) antigen 2.4384632000 S68616 Na+/H+ exchanger NHE-1 isom −2.5223464000 AB002318 KIAA0320 −2.4959950000 M27826 Endogenous retroviral protease −2.4913967000 HG2614-HT2710 Collagen Type Viii Alpha 1 2.3734545000 U12707 Wiskott-Aldrich syndrome protein (WASP); Also: U19927 2.3664510000 *U37408 CtBP 2.3356885000 X86691 218 kD Mi-2 protein −2.4076458000 U02619 TFIIIC Box B-binding subunit 2.2834708000 X99142 Hair keratin hHb6 2.2847916000 D26561 ORF E7 from papillomavirus 5b genome −2.4064124000 U35234 Protein tyrosine phosphatase sigma 2.2769785000 D11086 Interleukin 2 receptor gamma −2.3887671000 U22970 16-Jun (interferon-inducible peptide precursor); U22970 −2.3853381000 D31833 Vasopressin V1b receptor; Also: L37112 2.2463878000 S76475 TrkC from brain −2.3536759000 D63486 KIAA0152 2.2292978000 M96326 Azurocidin −2.3481101000 M91083 DNA-binding protein (HRC1) 2.2142609000 U23803 Heterologous ribonucleoprotein A0 2.2093005000 X54637 Tyk2 non-receptor protein tyrosine kinase 2.2109202000 J03600 Lipoxygenase −2.3282267000 Z11502 Intestine-specific annexin 2.1989181000 AB000895 Cadherin FIB1 −2.3181155000 M12125 Fibroblast muscle-type tropomyosin −2.3107464000 D49817 Fructose 6-phosphate 2-kinase/fructose 2 6-bisphosphatase 2.1814434000 D42085 KIAA0095 −2.3021685000 D49818 Fructose 6-phosphate 2-kinase/fructose 2 6-bisphosphatase 2.1724424000 M79463 PML-2; Also: HG560-HT560, M82827 −2.2904798000 U89336 Notch 4 −2.2881933000 Y08409 Spot14 −2.2876898000 S81737 Alpha 1 syntrophin; Also: U40571 2.1638767000 D10495 Protein kinase C delta-type 2.1579099000 U48861 Beta 4 nicotinic acetylcholine receptor subunit 2.1518600000 M97935 Transcription factor ISGF-3 sequence; M97935 −2.2592952000 U37219 Cyclophilin-like protein CyP-60 −2.2589364000 AC002077 Cosmid clone LUCA17/3p213 2.1358956000 Z78289 (clone 1D2)/Z78289 2.1371687000 D55640 Monocyte pseudoautosomal boundary-like sequence −2.2541249000 U31383 G protein gamma-10 subunit −2.2559957000 U15131 p126 (ST5) 2.1301085000 U31875 Hep27 protein −2.2477278000 X15331 Phosphoribosylpyrophosphate synthetase; D00860 2.1267157000 U65932 Extracellular matrix protein 1 (ECM1) −2.2467447000 X67325 p27 −2.2399248000 M38258 Retinoic acid receptor gamma 1 2.1084635000 D50855 Calcium-sensing receptor; Also: U20760, U20759 −2.2251800000 HG2036-HT2090 Stimulatory Gdp/Gtp Exchange protein C-Ki-Ras P21 −2.2257614000 U40223 Uridine nucleotide receptor (UNR) 2.1007323000 U68723 Checkpoint suppressor 1 2.1021763000 M25322 Granule membrane protein-140 −2.2175497000 M94345 Macrophage capping protein −2.2180100000 U89335 Notch 4 −2.2188636000 D78156 RasGTPase activating protein 2.0933341000 M33882 p78 protein −2.2166936000 X99728 NDUFV3/X99728 −2.2137169000 ***D16480 Mitochondrial enoylCoA hydratase 2.0832338000 Z49254 L23-related −2.2020794000 Z26256 L-type calcium channel/Z26256 2.0780216000 X53683 LAG-1 −2.1972116000 HG2175-HT2245 Myosin, Heavy Polypeptide 10, Non-Muscle; Also: M69181 2.0730215000 D28423 Pre-splicing factor SRp20 2.0701672000 D87078 KIAA0235 2.0722131000 HG162-HT3165 Tyrosine Kinase Receptor Axl 2 2.0712927000 L78833 Lfp35 from BRCA1, Rho7 and vatl 2.0703335000 X17651 Myf-4 myogenic determination factor −2.1869563000 X17254 TRANSCRIPTION FACTOR Eryf1 2.0632771000 HG3570-HT3773 Protein Phosphatase Inhibitor Homolog −2.1780412000 U63336 MHC Class I region proline rich protein −2.1787612000 X62573 RNA Fc receptor TC9 −2.1802693000 M27161 MHC class I CD8 alpha-chain (Leu-2/T8) −2.1755118000 M58597 ELAM-1 ligand fucosyltransferase (ELFT) −2.1774644000 S78085 PDCD2 = programmed cell death-2/Rp8 homolog −2.1691599000 D85939 p97 homolog 2.0528093000 U12139 Alpha1 (XI) collagen (COL11A1)/U12139 2.0572285000 U83843 HIV-1 Nef interacting protein (Nip7-1)/U83843 2.0546131000 X99350 HFH4 2.0568858000 Z48519 XG (clone RACE5)/Z48519; Also: Z48518 2.0560468000 U48707 Protein phosphatase-1 inhibitor −2.1658376000 U87964 Putative G-protein (GP-1) −2.1662080000 U03270 Centrin −2.1609185000 M96684 Pur (pur-alpha) 2.0450686000 U77968 Neuronal PAS1 (NPAS1) 2.0448728000 AF005037 Secretory carrier membrane protein (SCAMP1) −2.1531286000 M68864 ORF −2.1544240000 U24683 Anti-B cell autoantibody IgM heavy chain variable VDJ region 2.0397115000 X86018 MUF1 protein 2.0422801000 Z70220 Unknown protein (clone ICRFp507O0882)/Z70220 2.0423786000 HG1019-HT1019 Serine Kinase Psk-H1 −2.1511399000 HG3934-HT4204 G1 Phase-Specific −2.1499116000 L49169 G0S3 −2.1515997000 D49490 Disulfide isomerase-related protein −2.1380657000 D83783 KIAA0192 −2.1368790000 U45328 Ubiquitin-conjugating enzyme (UBE2I); Also: U31882 2.0229701000 M80563 CAPL protein −2.1310570000 M94167 Heregulin-beta2 2.0207548000 M63573 Secreted cyclophilin-like protein (SCYLP) 2.0167254000 D14827 Tax helper protein 1 −2.1194209000 L24774 Delta3, delta2-CoA-isomerase; Also: Z25821_rna1, Z25820 2.0109336000 V00551 Alpha interferon 2.0107027000 X12433 pHS1-2 with ORF homolog to membrane receptor proteins −2.1131910000 D42053 KIAA0091 2.0053307000 M58026 NB-1 2.0055666000 X93996 AFX prot 2.0044933000 U65011 Preferentially expressed antigen of melanoma (PRAME) −2.1092410000 D30755 KIAA0113 −2.1044871000 S83308 SOX5 = Sry-related HMG box 2.0011494000 Z18951 Caveolin 2.0024685000 Z48314 Apomucin; Also: U06711 1.9990217000 HG2290-HT2386 Calcitonin −2.1007151000 L42354 Clone 48ES4/L42354 −2.1001120000 M28825 Thymocyte antigen CD1a −2.0982975000 U40992 Heat shock protein hsp40 homolog 1.9974082000 U83192 Post-synaptic density protein 95 (PSD95) 1.9959202000 X70218 Protein phosphatase X 1.9929730000 Y08263 AAD14 protein −2.0928083000 S34389 Heme oxygenase-2 [kidney 1627 nt] −2.0891099000 L43579 Clone 110298/L43579; Also: L43575 1.9857183000 M80647 Thromboxane synthase 1.9832428000 Z31695 43 kDa inositol polyphosphate 5-phosphatase 1.9831751000 L38487 Estrogen receptor-related protein (hERRa1) −2.0839503000 D50402 NRAMP1 1.9797759000 *M94250 Retinoic acid inducible factor (MK) 1.9788194000 *X64072 CD18; Also: M15395 1.9817507000 X93499 RAB7 prot 1.9775636000 J05582 Pancreatic mucin; Also: J05581 1.9740898000 S66431 RBP2 = retinoblastoma binding protein 2 1.9738895000 U04343 CD86 antigen −2.0770043000 X62153 P1 protein (P1.h); Also: D38073 −2.0763673000 X79066 ERF-1 −2.0739931000 AB000409 MNK1 −2.0695756000 J02947 Extracellular-superoxide dismutase (SOD3); Also: U10116 1.9665406000 M30185 Cholesteryl ester transfer protein −2.0591846000 U31384 G protein gamma-11 subunit −2.0615467000 M23294 Beta-hexosaminidase beta-subunit (HEXB) 1.9578227000 U18235 ATP-binding cassette protein (ABC2) HFBCD04 clone 1.9605421000 HG3731-HT4001 Ig Heavy Chain, Vdjrc Regions L23566 1.9552306000 M54951 Atrial natriuretic factor 1.9556397000 U20428 SNC19 sequence 1.9529377000 X63755 High-sulphur keratin 1.9523322000 X79483 ERK6 extracellular signal regulated kinase 1.9481684000 AF001294 IPL −2.0447357000 U16031 TRANSCRIPTION FACTOR IL-4 Stat −2.0447357000 X98833 Zinc finger protein, Hsal1 −2.0473722000 J04948 Alkaline phosphatase (ALP-1) 1.9444086000 X04898 Apolipoprotein All 1.9464474000 X52896 Dermal fibroblast elastin; Also: HG2994-HT4851 1.9470905000 X56199 XIST a (locus DXS399E) 1.9455917000 X90872 gp25L2 protein 1.9451524000 HG4757-HT5207 Oncogene MII-Af4, Fusion Activated; Also: L13773 −2.0424771000 U33839 Potassium channel/U33839 −2.0417873000 X99140 Hair keratin hHb5 1.9380942000 D88155 DNA for Ad4BP (SF-1); Also: U76388 −2.0367287000 M68840 Monoamine oxidase A (MAOA) 1.9351040000 U58032 Myotubularin related protein 1 (MTMR1)/U58032 1.9342459000 X70683 SOX-4 protein 1.9370161000 D82060 Kidney histidine rich putative membrane protein −2.0292823000 J04056 Carbonyl reductase −2.0295867000 S73813 CD39 = lymphoid cell activation antigen −2.0275535000 AF002224 E6-AP ubiquitin protein ligase 3A/promoter P1 1.9280628000 U13369 Ribosomal DNA repeating unit/U13369 1.9283702000 M19888 Small proline rich protein (sprl), clone 128 −2.0258177000 U63455 Sulfonylurea receptor (SUR1) −2.0264311000 X69433 Mitochondrial isocitrate dehydrogenase (NADP+) −2.0251010000 X13293 B-myb 1.9241500000 X71490 Vacuolar proton ATPase subunit D 1.9232699000 D84239 IgG Fc binding protein −2.0197392000 L03840 Fibroblast growth factor receptor 4 (FGFR4); Also: X57205 −2.0213543000 *U57971 Calcium ATPase isoform 3x/a; Also: U60414 −2.0217060000 X68688 ZNF33B; Also: D31763 −2.0095571000 X16260 Inter-alpha-trypsin inhibitor subunit 3; Also: X69532_rna1 1.9108378000 U05040 FUSE binding protein −2.0033528000 U83303 GCP-2 (granulocyte chemotactic protein-2) −2.0065730000 X96698 D1075-like −2.0043214000 HG2188-HT2258 Paired Box Hup1 1.9040931000 M55621 N-acetylglucosaminyltransferase I (GlcNAc-TI) 1.9061195000 *M85220 Heavy chain disease IgA chain CH3 region 1.9073097000 M92424 p53 associated MDM2 −1.9992393000 M76732 HOX7; Also: M97676 1.8986155000 M98447 Keratinocyte transglutaminase −1.9956352000 U71364 Serine protase inhibitor (P19) −1.9973864000 Y10514 CD152 protein/Y10514; Also: Y10508 −1.9929951000 D88146 UDP-galactose transporter 2 1.8931108000 U00928 Clone CE29 4.1 (CAC)n/(GTG)n repeat-containing 1.8961954000 U29615 Chitotriosidase precursor 1.8968843000 L05188 Small proline-rich protein 2 (SPRR2B) −1.9881128000 D13988 Rab GDI 1.8898058000 M88282 Tactile protein −1.9848647000 Z22548 Thiol-specific antioxidant protein −1.9789790000 D87937 Alpha(1,2)fucosyltransferase 5 −1.9756311000 X78338 Synthetic adenovirus transformed retinal cell line MRP −1.9770373000 HG3502-HT3696 Homeotic protein Hox54 1.8756978000 U33920 Clone lambda 5 semaphorin 1.8739306000 X82207 Beta-centractin (PC3) −1.9657895000 U07882 Delta opioid receptor 1.8667303000 Y07565 RIN protein; Also: U71204 1.8655777000 AB000462 SH3 binding RES4-23A −1.9614270000 HG3921-HT4191 Homeotic protein C6, Class I −1.9577270000 J03909 Gamma-interferon-inducible protein (IP-30) −1.9586833000 K02882 IGHD (Ig delta-chain); Also: K02882_2 −1.9580858000 U78180 Sodium channel 2 (hBNaC2) −1.9604708000 U15197 Histo-blood group ABO protein 1.8577545000 D88795 Cadherin −1.9559282000 M21984 (clone PWHTnT16) skeletal muscle Troponin T −1.9555675000 U37248 Alpha-mannosidase (6A8) −1.9553269000 X66401 LMP2 from TAP1, TAP2, LMP2, LMP7 and DOB −1.9525503000 Z29083 5T4 Oncofetal antigen −1.9550862000 M37075 Embryonic/atrial myosin light chain (MLC-1-emb/A isoform) 1.8536982000 U32576 Apolipoprotein apoC-IV (APOC4) −1.9517017000 HG4557-HT4962 Small Nuclear Ribonucleoprotein U1, 1snrp 1.8495730000 L20859 Leukemia virus receptor 1 (GLVR1) 1.8480315000 L35240 Enigma −1.9442358000 M21389 Keratin type II (58 kD) −1.9454686000 U07919 Aldehyde dehydrogenase 6 −1.9452223000 U28687 Zinc finger containing protein ZNF157 (ZNF157) −1.9474337000 U52154 G protein-coupled inwardly rectifying K+ channel Kir34 −1.9444827000 X07695 Cytokeratin 4 −1.9460836000 X89101 Fas (Apo-1, CD95)/X89101; Also: X83493, X63717, X83492 −1.9459607000 L40393 Clone S171 1.8411404000 M59916 Acid sphingomyelinase (ASM) 1.8401061000 M58603 Nuclear factor kappa-B DNA binding subunit (NF-kappa-B) −1.9367650000 U02632 Calcium-activated potassium channel −1.9338668000 L05500 Fetal brain adenylyl cyclase 1.8354686000 L37199 Clone cD24-1 Huntington's candidate region fragment 1.8371147000 S46622 Calcineurin A catalytic subunit 1.8343889000 U09411 Zinc finger protein ZNF 132 −1.9281397000 U37519 Aldehyde dehydrogenase (ALDH8) −1.9301847000 U80184 FLII 1.8287565000 L27071 Tyrosine kinase (TXK) 1.8251339000 X94453 Pyrroline 5-carboxylate synthetase 1.8253937000 D79985 KIAA0163 −1.9194703000 M54968 K-ras onco protein −1.9203842000 U05340 p55CDC −1.9212962000 U38480 Retinoid X receptor-gamma −1.9189473000 *M13241 N-myc 1.8188182000 M13981 Inhibin A-subunit 1.8177636000

[0034] TABLE 10 Gene targets in heterogeneous MS spinal cord gray matter specimens. Probe sets Gene descriptions Up (+) or down (−) U70063 Acid ceramidase + X65644 MBP-2 MHC binding protein 2 + X71129 Electron transfer flavoprotein beta subunit − L07515 Heterochromatin protein homolog (HP1) − U82671 HSP1-A from cosmids from Xq28 − D49958 Membrane glycoprotein M6 + X95404 Non-muscle type cofilin − **D78014 Dihydropyrimidinase related protein-3 + X05997 Gastric lipase − M64108 Udulin 1 − L48546 Tuberin (TSC2) − AB000381 GPI-anchored molecule-like, also D84290 − D89859 Zinc finger 5 protein − *D10704 Choline kinase + *X64072 CD18; Also: M15395 + X13916 LDL-receptor related protein + U37690 RNA polymerase II subunit (hsRPB10) − U12404 Csa-19 − D13900 Mitochondrial short-chain enoyl-CoA hydratase − X62654 ME491/CD63 antigen + U34605 Retinoic acid- and interferon-inducible 58 K prot RI58 − M15395 Leukocyte adhesion protein (LFA-1/Mac-1) beta subunit + U20530 Bone phosphoprotein spp-24 precursor/U20530 − U49785 D-dopachrome tautomerase − M76378 Cysteine-rich protein (CRP) − L19437 Transaldolase containing transposable element − X79683 Z68155 and others + M34079 HIV tat transactivator binding protein-1 (tbp-1) − U15197 Histo-blood group ABO protein + X69433 Mitochondrial isocitrate dehydrogenase (NADP+) − M58286 TNF receptor; Also: M63121, M33294, X55313, M75866 + U58090 Hs-cul-4A + U01317 Beta-globin thalassemia from beta globin region − M92449 Human LTR − U09564 Serine kinase − U48437 Amyloid precursor-like protein 1 − AC000099 Cosmid g0771a003 − S95936 Transferrin − D26598 Proteasome subunit HsC10-II − D83243 NPAT − U06452 Melanoma antigen recognized by T-cells (MART-1) − U90716 Cell surface protein HCAR − X78992 ERF-2 + U82256 Arginase type II − M35252 CO-029 − J03068 DNF1552 (lung) + M64231 Spermidine synthase − HG1471-HT3923 Transcription Factor Oct-1a/1b; Also: X13403 − L17131 High mobility group protein HMG-I(Y) + U94332 Osteoprotegerin (OPG) − U53204 Plectin (PLEC1) + U32581 Lambda/iota-protein kinase C-interacting protein − D78151 26S proteasome subunit p97 − U59877 Low-Mr GTP-binding protein (RAB31); Also: U57091 + U49974 Mariner2 transposable element/U49974 − X99687 Methyl-CpG-binding protein 2 intron 2/X99687 − AB002356 KIAA0358; Also: U77352 + M75106 Prepro-plasma carboxypeptidase B − X99720 TPRC + U58675 Olfactory receptor cluster + L13800 Liver expressed protein/L13800 − *D38583 Calgizzarin + L10413 Farnesyltransferase alpha-subunit − D82344 NBPhox − D38555 KIAA0079 +

[0035] TABLE 11 Gene targets in heterogeneous MS spinal cord white matter specimens Probe sets Gene descriptions Up (+) or down (−) Y09321 TAFII105 − M15465 Pyruvate kinase type L; Also: D13243 − U16120 Placental taurine transporter; Also: Z18956 − U34976 Gamma-sarcoglycan − U53442 p38Beta MAP kinase − HG3570-HT3773 Protein Phosphatase Inhibitor Homolog − Z11793 Selenoprotein P − Z48501 Polyadenylate binding protein II/Z48501; Also: U68105 + D28532 Renal Na+-dependent phosphate cotransporter − D28114 Myelin-associated oligodendrocytic basic protein − X69908 Mitochondrial ATP synthase c subunit (P2 form) − X92814 Rat HREV107-like protein − M62958 R degradation slow (RDS) − U40763 Clk-associated RS cyclophilin CARS-Cyp; Also: X99717 − D00723 Hydrogen carrier protein − D90282 Carbamyl phosphate synthetase I − M73077 Glucocorticoid receptor repression factor 1 (GRF-1) − D87953 RTP − X15675 pTR7 repetitive sequence/X15675 − AF009674 Axin − U06698 Neuronal kinesin heavy chain − AF000545 Putative purinergic receptor P2Y10 − M20471 Brain-type clathrin light-chain a − AB000468 Zinc finger protein RES4-26 − X00368 Prolactin 5/X00368 − X97074 mRNS clathrin-associated protein − D90224 gp34 − L11695 Activin receptor-like kinase (ALK-5) − M26880 Ubiquitin − X51602 Flt receptor-related tyrosine kinase − D00763 Proteasome subunit HC9 − D38498 PMS5 (yeast PMS1 homolog) − U37690 RNA polymerase II subunit (hsRPB10) − X12530 B lymphocyte antigen CD20 (B1, Bp35); Also: X07203 − D13413 Tumor-associated 120 kDa nuclear protein p120 − Y00264 Amyloid A4 precursor of Alzheimer's disease − L19437 Transaldolase containing transposable element − L77864 Stat-like protein (Fe65) − Y10262 EYA3/Y10262; Also: U81602 − X66534 Soluble guanylate cyclase large subunit − X04706 Homeobox (clone HHO.c13); Also: X17360_rna1 − D79205 Ribosomal protein L39 − HG3495-HT3689 Collagen Type Ix Alpha 1 − U28369 Semaphorin V − U91618 Proneurotensin/proneuromedin N − L20941 Ferritin heavy chain − S59184 RYK = related to receptor tyrosine kinase − X17622 HBK2 potassium channel protein − X17025 Homolog of yeast IPP isomerase − U83461 Putative copper uptake protein (hCTR2)/U83461 − U37359 MRE11 homolog hMRE11 − U13395 Oxidoreductase (HHCMA56) − L07548 Aminoacylase-1 (ACY1) − U19247 Interferon-gamma receptor alpha chain + U11877 Interleukin-8 receptor type B (IL8RB)/U11877 − M84605 Putative opioid receptor − M90657 Tumor antigen (L6) − M79462 PML-1 − U28687 Zinc finger containing protein ZNF157 (ZNF157) − M13929 c-myc-P64; Also: HG3523-HT4900, HG3523-HT4899 − M64929 Protein phosphatase 2A alpha subunit + HG2815-HT4023 Myosin, Light Chain/U02629; Also: HG2815-HT1357 − Z50853 CLPP − L43338 Cadherin/L43338 − U48959 Myosin light chain kinase (MLCK) − HG1614-HT1614 Protein Phosphatase 1 Alpha Catalytic Subunit − D17716 N-acetylglucosaminyltransferase V − Y00636 Lymphocyte function associated antigen-3 (LFA-3) − M27826 Endogenous retroviral protease − U32576 Apolipoprotein apoC-IV (APOC4) − L47276 Alpha topoisomerase/L47276; Also: L47277 − L14787 DNA-binding protein − D63880 KIAA0159 − U41060 Breast cancer estrogen regulated LIV-1 protein (LIV-1) − M62762 Vacuolar H+ ATPase proton channel subunit − D10922 FMLP-related receptor (HM63)-Also: M84562 − M21984 Skeletal muscle Troponin T − **HG1877-HT1917 Myelin Basic protein; Also: M13577 + X13546 Putative HMG-17 non-histone protein + HG2465-HT4871 Dna-Binding protein Ap-2 3 − L03840 Fibroblast growth factor receptor 4 (FGFR4); X57205 − U07151 GTP binding protein (ARL3) − Z68129 H-IDH NADH isocitrate dehydrogenase gamma − U69126 FUSE binding protein 2 (FBP2); Also: U94832 − D50863 TESK1 − AB002382 KIAA0384 − X01703 Alpha-tubulin (b alpha 1) − L35249 Vacuolar H+-ATPase Mr 56,000 subunit (HO57); M60346 + L36818 (clone 51C-3) 51C protein − L25119 Mu opiate receptor (MOR1) − M12125 Fibroblast muscle-type tropomyosin − X15822 COX VIIa-L liver-specific cytochrome c oxidase − M97347 Beta-1,6-N-acetylglucosaminyltransferase; L41415 − D87258 Cancellous bone osteoblast serin protease − X95240 Cysteine-rich secretory protein-3; Also: X94323 − D86962 KIAA0207 − M57703 Melanin concentrating hormone (MCH); Also: S63697 − X02874 (2′-5′) oligo A synthetase E − L76159 FRG1 − AB000220 Semaphorin E − M99487 Prostate-specific membrane Antigen − D85758 DROER homolog + X54637 Tyk2 non-receptor protein tyrosine kinase + U89335 Notch 4 − X14684 La protein C-terminal region; Also: X13697, M20328 − X99975 hRTR/hGCNF protein − AF005043 Poly(ADP-ribose) glycohydrolase (hPARG) − X76132 DCC − U50527 BRCA2 region, sequence CG018; Also: U57962 − X74330 DNA primase (subunit p48) − M96326 Azurocidin − X55889 Ciliary neurotrophic factor 1 − D28791 PIG-A − D78367 K12 keratin − D79997 KIAA0175 − U02082 Guanine nucleotide regulatory protein (tim1) − AF001294 IPL − X63629 P cadherin − D82060 Kidney histidine rich putative membrane protein − D14822 CBFA2T1 − D38437 DNA mismatch repair − M25322 Granule membrane protein-140 − M84424 Cathepsin E (CTSE) − *M54927 Myelin proteolipid protein − X57351 1-8D from interferon-inducible family; HG1538-HT1538 − U00952 Clone A9A2BRB7 (CAC)n/(GTG)n repeat-containing + D31766 KIAA0060 + U03057 Actin bundling protein (HSN) − U65932 Extracellular matrix protein 1 (ECM1) − S87759 Protein phosphatase 2C alpha − HG2059-HT2114 Arrestin Beta 2 − X77584 ATL-derived factor/thiredoxin + HG651-HT4201 Adducin Alpha Subunit 2 + L10374 (clone CTG-A4) sequence − X85785 DARC − L77886 Protein tyrosine phosphatase − HG1980-HT2023 Tubulin, Beta 2 − U28963 Gps2 (GPS2) + U78180 Sodium channel 2 (hBNaC2) − X78136 hnRNP-E2 + X73460 Ribosomal protein L3 + X60188 ERK1 protein serine/threonine kinase − M14058 Complement C1r − D30756 KIAA0049 − U66061 TCRBC1 from germline T-cell receptor beta chain − X66436 Hsr1 − X77753 TROP-2 − U06233 POU domain protein (Brn-3b) − D28915 Hepatitis C-associated microtubular aggregate p44 − M94556 mitochondrial specific ss-DNA binding protein − HG1019-HT1019 Serine Kinase Psk-H1 − X66079 Spi-B + D83243 NPAT − HG846-HT846 Cyclophilin-Related protein − X96753 Melanoma-associated chondroitin sulfate proteoglycan − M13903 Involucrin + M13232 Factor VII serine protease precursor; Also: J02933 − **L40027 Glycogen synthase kinase 3 − Y00757 Polypeptide 7B2 − U22398 Cdk-inhibitor p57KIP2 (KIP2) − L16464 ETS onco (PEP1) − U63336 MHC Class I region proline rich protein − M81601 Transcription elongation factor (SII) + AB000114 Osteomodulin − X83929 Type 3 desmocollin; Also: D17427 − S73813 CD39 = lymphoid cell activation antigen − U37219 Cyclophilin-like protein CyP-60 − V00594 Metallothionein from cadmium-treated cells; J00271 − D83542 Cadherin-15 − M31520 Ribosomal protein S24; Also: HG3214-HT3391 − U04343 CD86 antigen − X06272 Docking protein (signal recognition particle receptor) + U38964 PMS2 related (hPMSR2); Also: D38502 − D31765 KIAA0061 − D50477 Membrane-type matrix metalloproteinase 3; D83646 − U51477 Diacylglycerol kinase zeta − X69920 Calcitonin receptor; Also: L00587 − *D90086 Pyruvate dehydrogenase beta subunit − U41816 C-1 − X05130 Prolyl 4-hydoxylase beta subunit; Also: J02783 + AB000895 Cadherin FIB1 − *D63135 ETS-like 30 kDa prot − U50330 Procollagen C-protase (pCP-2) − X89894 Nuclear receptor − U01691 Annexin V (ANX5) 5-UTR; Also: X12454, M18366 + U49957 LIM protein (LPP); Also: U49968 − D21851 KIAA0028 − HG4704-HT5146 Glial Growth Factor 2 − D55640 Monocyte pseudoautosomal boundary-like sequence − D63874 HMG-1 − L23333 Corticotropin releasing factor receptor; Also: X72304 + U15131 p126 (ST5) + M83088 Phosphoglucomutase 1 (PGM1) − L42379 Bone-derived growth factor (BPGF-1) − AF005037 Secretory carrier membrane protein (SCAMP1) − J02947 Extracellular-superoxide dismutase (SOD3) + U12707 Wiskott-Aldrich syndrome protein (WASP); Also: U19927 + Y10204 CD77 protein/Y10204 − U19906 Arginine vasopressin receptor 1 (AVPR1) − HG3175-HT3352 Carcinoembryonic Antigen − X15306 NF-H 1 − D63851 Unc-18 homolog − X64707 BBC1 − M87339 Replication factor C 37-kDa subunit + X86809 Major astrocytic phosphoprotein PEA-15 − J04164 Interferon-inducible protein 27-Sep − D14878 Protein D123 − M93311 Metallothionein-III − U04520 Type IV collagen a5 chain (COL4A5) − X71129 Electron transfer flavoprotein beta subunit − L14837 Tight junction (zonula occludens) protein ZO-1 + D16469 ORF Xq terminal portion − L11372 Protocadherin 43 − X02751 N-ras − J03824 Uroporphyrinogen III synthase + S67798 PH-20 − U16031 TRANSCRIPTION FACTORS IL-4 Stat − L43964 (clone F-T03796) STM-2 − U79526 Orphan G-protein coupled receptor Dez isoform a − L10413 Farnesyltransferase alpha-subunit − HG3432-HT3621 Fibroblast Growth Factor Receptor K-Sam − M57466 MHC class II HLA-DP light chain; Also: M83664, X00532 + D63876 KIAA0154 − U07794 Tyrosine kinase (TXK) − X13839 Vascular smooth muscle alpha-actin − X07290 HF12 − HG2264-HT2360 Atpase Ca2+ Transporting Plasma Membrane 1 6 − U11037 Sel-1 like + D63475 KIAA0109 − U44754 PSE-binding factor PTF gamma subunit − L78132 Prostate carcinoma tumor antigen (pcta-1) − D86977 KIAA0224 − U83192 Post-synaptic density protein 95 (PSD95) + M21142 Guanine nucleotide-binding protein G-s-alpha-3; M21142 + L41067 NF-AT4c − D26561 ORF E7 from papillomavirus 5b genome − U59111 Dermatan sulfate proteoglycan 3 (DSPG3) − HG2999-HT4756 Thyroid Peroxidase; Also: M25715 + M62403 Insulin-like growth factor binding protein 4 (IGFBP4) − AB000115 Unknown protein − D90276 CGM7 nonspecific cross-reacting antigen (NCA) − M76424 Carbonic anhydrase VII (CA VII) + D31762 KIAA0057 − L76568 S26 from excision and cross link repair protein (ERCC4) − X57579 Activin beta-A subunit (2); Also: J03634 + X02404 Second calcitonin related peptide (CGRP) − Y10936 Hypothetical protein downstream of DMPK and DMAHP − D13643 KIAA0018 − AF005361 Importin alpha 6 − U41737 Pancreatic beta cell growth factor (INGAP)/U41737 − K01383 Metallothionein-I-A − D80008 KIAA0186 − AB002533 Qip1 − U68135 SCC-S1c expressed in squamous cell cancer/U68135 − X79353 XAP-4 GDP-dissociation inhibitor − D50310 Cyclin I + D15049 Protein tyrosine phosphatase − U31930 Deoxyuridine nucleotidohydrolase − M55543 Guanylate binding protein isom II (GBP-2) − M31303 Oncoprotein 18 (Op18) − U45328 Ubiquitin-conjugating enzyme (UBE2I); Also: U31882 + L34657 Platelet/endothelial cell adhesion molecule-1 (PECAM-1) + U33818 Inducible poly(A)-binding protein + M16653 Pancreatic elastase IIB − U63825 Hepatitis delta antigen interacting protein A (dipA) − AB002318 KIAA0320 − X66276 Skeletal muscle C-protein; Also: X73114 − D13631 KIAA0006; Also: D25304 + M91467 Serotonin receptor (5HT1E) − Z56281 Interferon regulatory factor 3 − M37238 Phospholipase C; Also: X14034 + X81003 HCG V − J00277 Lambda-[SK2-T2, HS578T]; RS-[3, 4, 6]) c-Ha-ras1 − L42373 Protein phosphatase 2A B56-alpha − J00210 IFNA (interferon alpha-d) − HG3523-HT4899 Proto-Oncogene C-Myc; Also: L00058, HG3523-HT4900 + AF001548 815A9.1 myosin heavy chain from chromosome 16 − L24774 Delta3, delta2-CoA-isomerase; Also: Z25821 + Z48054 Peroxisomal targeting signal 1 (SKL type) receptor − D13720 LYK; Also: L10717 − D87453 KIAA0264 −

[0036] TABLE 12 Gene targets found across all comparisons of MS gray matter spinal cord tissues against normal gray matter spinal cord tissues.* Probe Set Gene description Mean fold change Mean P value *M87789 Hybridoma H210 3.0601579 0.000696592 anti-hepatitis A IgG V, C, CDR regions *X64072 CD18; Also: M15395 1.8796121 0.00822973 M13207 Granulocyte-macrophage −2.063521 0.012103845 colony-stimulating factor (CSF1) HG2709- Serine/Threonine Kinase 1.6333372 0.016343018 HT2805 M16707 Histone H4; clone FO108 −1.9707812 0.019372876

[0037] TABLE 13 Gene targets found across all comparisons of MS white matter spinal cord tissues against normal white matter spinal cord tissues. Probe Set Gene description Mean fold change Mean P value M84739 Autoantigen calreticulin 2.6243939 0.003487238 AB000895 Cadherin FIB1 −2.3163955 0.0055741 U12707 Wiskott-Aldrich syndrome protein (WASP); Also: U19927 2.2626829 0.005747785 *M63438 Ig rearranged gamma chain , V-J-C region; Also: X96754 3.0521967 0.006442657 U35234 Protein tyrosine phosphatase sigma 2.2824217 0.007725067 U37219 Cyclophilin-like protein CyP-60 −2.2580722 0.007876164 U45328 Ubiquitin-conjugating enzyme (UBE2I); Also: U31882 2.2253883 0.008423851 *M87789 Hybridoma H210 anti-hepatitis A IgG V, C, CDR regions 2.6095958 0.010125314 J02947 Extracellular-superoxide dismutase (SOD3) 2.1364149 0.012132355 X54637 Tyk2 non-receptor protein tyrosine kinase 2.0976451 0.012253421 *U37408 CtBP 2.09237 0.014673944 L24774 Delta3, delta2-CoA-isomerase; Also: Z25821_rna1 2.0763149 0.014787034 HG3033-HT3194 Spliceosomal protein Sap 62 2.2991536 0.015744522 U15131 p126 (ST5) 2.040288 0.016092199 *X64072 CD18; Also: M15395 2.0389044 0.018208883 HG162-HT3165 Tyrosine Kinase Receptor Axl 2 2.0291313 0.018333948 X15331 Phosphoribosylpyrophosphate synthetase subunit one 2.0054747 0.018860938 M96684 Pur (pur-alpha) 2.0364039 0.022166073 M23294 Beta-hexosaminidase beta-subunit (HEXB) 1.9720603 0.024128352 D42053 KIAA0091 1.9407077 0.024673169 U71364 Serine protase inhibitor (P19) −1.9973864 0.026455898 U83192 Post-synaptic density protein 95 (PSD95) 1.8968397 0.026959056 M21984 (clone PWHTnT16) skeletal muscle Troponin T −1.9555675 0.030792454

[0038] TABLE 14 Gene targets found across all comparisons of MS vs. normal spinal cord tissues, including gray and white matter comparisons. Probe Set Gene description Mean fold change Mean P value *M87789 Hybridoma H210 2.809845633 0.005934771 anti-hepatitis A IgG V, C, CDR regions *X64072 CD18; Also: M15395 1.968107833 0.013773704

[0039] TABLE 15 MS target genes commonly altered across MS spinal cord white matter samples that contain inflammatory cells and have evidence of demyelination. Probe set Gene description Mean fold change Mean P value *M63438 Ig rearranged gamma chain, V-J-C region; Also: X96754 3.1649421 0.00019838 *M87789 Hybridoma H210 anti-hepatitis A IgG V, C, CDR regions 2.6612373 0.001353321 D26561 ORF E7 from papillomavirus 5b genome −2.4064124 0.003085073 U22970 16-Jun (interferon-inducible peptide precursor) −2.3853381 0.003506211 M84739 Autoantigen calreticulin 2.3988885 0.005304639 AB000895 Cadherin FIB1 −2.3152488 0.005469599 U45328 Ubiquitin-conjugating enzyme (UBE2I); Also: U31882 2.2473988 0.005664919 U12707 Wiskott-Aldrich syndrome protein (WASP); Also: U19927 2.236641 0.006397345 J04948 Alkaline phosphatase (ALP-1) 2.2390081 0.007089837 U37219 Cyclophilin-like protein CyP-60 −2.257496 0.0076284 J02947 Extracellular-superoxide dismutase (SOD3); U10116 2.1735344 0.008235838 X67325 p27 −2.2399248 0.00837286 U35234 Protein tyrosine phosphatase sigma 2.2315119 0.010160845 L41143 Expressed pseudo TCTA at t(1;3) translocation site 2.2002311 0.010868089 U12139 Alpha1(XI) collagen (COL11A1)/U12139 2.1197746 0.010952425 X54637 Tyk2 non-receptor protein tyrosine kinase 2.1068855 0.011617197 HG3033-HT3194 Spliceosomal protein Sap 62 2.3472607 0.012248234 HG162-HT3165 Tyrosine Kinase Receptor Axl 2 2.1075667 0.012419809 *X64072 CD18; Also: M15395 2.1152978 0.0127252 HG3945-HT4215 Phospholipid Transfer protein 2.3308357 0.013077384 U02619 TFIIIC Box B-binding subunit 2.2199388 0.013347355 X95406 Cyclin E −2.1339379 0.013951429 L24774 Delta3, delta2-CoA-isomerase; Also: Z25821 2.0417176 0.015024809 M28825 Thymocyte antigen CD1a −2.0982975 0.016299644 *U37408 CtBP 2.0620477 0.01643724 M23294 Beta-hexosaminidase beta-subunit (HEXB) 2.0583126 0.017046586 X07315 PP15 (placental protein 15) 2.0088193 0.017057852 D42053 KIAA0091 2.00626 0.017700929 U15131 p126 (ST5) 2.010507 0.018236373 U15655 Ets domain protein ERF 1.9931435 0.020560907 M61199 Cleavage signal 1 protein 1.981728 0.021409014 X93996 AFX protein 2.050328 0.023466008 X15331 Phosphoribosylpyrophosphate synthetase subunit one 1.926366 0.024012526 Z26256 L-type calcium channel 1.9508756 0.02443943 M36429 Transducin beta-2 subunit; Also: M16538 1.9340099 0.024855746 U71364 Serine protase inhibitor (P19) −1.9973864 0.025176509 U83192 Post-synaptic density protein 95 (PSD95) 1.8899076 0.026517609 U33920 Clone lambda 5 semaphorin 1.8937119 0.028148796 U27333 Alpha (1,3) fucosyltransferase (FUT6), major transcript I 1.8809063 0.028243361 M96684 Pur (pur-alpha) 1.9775652 0.028255093 M21984 Clone PWHTnT16 skeletal muscle Troponin T −1.9555675 0.029442849

[0040] TABLE 16 Genes previously reported to be dysregulated in MS central nervous system tissues.* Probe set Gene description Up (+) or down (−) U89606 Pyridoxal kinase + D10704 Choline kinase + X05610 Type IV collagen alpha-2 chain + M87789 Hybridoma H210 anti-hepatitis A IgG V, C, CDR regions + U18919 Chromosome 17q12-21 clone pOV-2 + U16031 TRANSCRIPTION FACTOR IL-4 Stat + HG1595-HT4788 Heterogeneous Nuclear Ribonucleoprotein I; HG1595-HT4789 + U21090 DNA polymerase delta small subunit + L26339 Autoantigen + U62317 Hypothetical protein 384D8_7 + D38583 Calgizzarin + M13241 N-myc + L25270 XE169 + U37408 CtBP + M63438 Ig rearranged gamma chain, V-J-C region; Also: X96754 + L05624 MAP kinase kinase; Also: L11284 + U52518 Grb2-related adaptor protein (Grap) + U64573 Connexin43 gap junction prot (connexin43)/U64573 + M35999 Platelet glycoprotein IIIa (GPIIIa) + X13334 CD14 myeloid cell-specific leucine-rich glycoprotein + M94250 Retinoic acid inducible factor (MK) + M85220 Heavy chain disease IgA chain CH3 region + X57809 Rearranged Ig lambda light chain; S42404 + HG2730-HT2828 Fibrinogen, A Alpha Polypeptide; Also: M58569 + D84145 WS-3 − M11749 Thy-1 glycoprotein − U28811 Cysteine-rich fibroblast growth factor receptor (CFR-1) − S82024 SCG10 = neuron-specific growth-associated protein/stathmin homolog − M74826 Glutamate decarboxylase (GAD-2) − D90086 Pyruvate dehydrogenase beta subunit − D61391 Phosphoribosypyrophosphate synthetase-associated protein 39 − X00734 Beta-tubulin (5-beta) with ten Alu family members − U57971 Calcium ATPase isoform 3x/a; Also: U60414 − M54927 Myelin proteolipid protein − X63578 Parvalbumin − X07109 Protein kinase C (PKC) type beta II − D63135 ETS-like 30 kDa protein − J03263 Lysosome-associated membrane glycoprotein (lamp A) − D13988 Rab GDI − M58459 Ribosomal protein (RPS4Y) isom − U60269 Putative ERVK envelope protein − Y12711 Putative progesterone binding protein − #for some of these genes (i.e., Ig lambda light chain and Heavy chain disease IgA chain CH3 region) were not mentioned in the report by Lock et al. (2002). The probe set identifier for fibrinogen (HG2730-HT2828) was not identical to the probe set in the report by Lock et al. (2002) (HG2730-HT2827).

[0041] TABLE 17 Genes previously reported to be dysregulated in MS brain lesions using high throughput sequencing of cDNA libraries (Chabas et al., Science 2001; 294: 1731-5) and also shown by the inventors to be similarly dysregulated in MS spinal cords, using DNA microarrays.** Up (+) Probe set Gene Name or Down (−) D78014 Dihydropyrimidinase related protein-3 + HG1877-HT1917 Myelin Basic Protein + X05299 Major centromere autoantigen CENP-B + L40027 Glycogen synthase kinase 3 − #3 shares the probe set number identifier with the report by Chabas et al. (2001). The designation HG1877-HT1917 is a probe set identifier provided by Affymetrix. The probe set identifiers for Major centromere autoantigen CENP-B (X05299) and Glycogen synthase kinase 3 (L40027) are not identical to those reported by Chabas et al. for these genes.

[0042] TABLE 18 Genes previously reported to be dysregulated in MS brain lesions using filter cDNA microarrays (Whitney et al., Annals of Neurology, 1999; 46(3): 425-8), and also shown by the inventors to be similarly dysregulated in MS spinal cords, using DNA microarrays.*** Probe set Gene Name Up (+) or Down (−) D16480 Mitochondrial enoylCoA hydratase + J05037 Serine dehydratase + #reported by Whitney et al. (1999) (75860 for Mitochondrial enoylCoA hydratase and 76751 for serine dehydratase) differ from the probe set identifiers shown above.

[0043] III. Gene Therapy

[0044] Thus, in accordance with the present invention, there are provided methods for the treatment of MS by gene therapy. Such methods include both the administration of a gene therapy vector encoding one or more genes identified as being downregulated in MS, and for genes that are overexpressed in MS, transgenes may be provided that reduce expression of appropriate targets.

[0045] MS is an inflammatory disease of the central nervous system. Entry of immune cells into the perivascular tissues of the brain and spinal cord lead to loss of myelin and eventually to axonal loss and neurodegeneration. In some cases, axonal loss occurs during the early stages of formation of the MS lesions. The molecules that mediate this tissue damage (i.e., from activated immune cells or from the affected tissues themselves) can be targeted with various therapies, to attempt to revert the ongoing demyelination or loss of axons. For instance, in Table 1, multiple genes are found to have elevated expression in MS tissues. Glutamate excitotoxicity has been linked to MS. Excitatory amino acid transporters and receptors, as well as calcium entry into the cells mediated by calcium channels, are mechanisms involved in glutamate toxicity. The metabotropic glutamate receptor 4 (probe set U92457) and the excitatory amino acid transporter 4 (U18244) are found to be elevated. Similarly, the P/Q-type calcium channel alpha 1 subunit was elevated. Among the inflammatory genes that are found to be elevated, complement component 2 (L09708), Ig-like transcript 2 (U82279), interleukin 8 receptor type B (U11877), Ig heavy chain VDJC region (HG4458-HT4727), monocyte chemoattractant protein-4 precursor (U46767), phospholipase A2 (M21056), granulocyte colony-stimulating factor receptor (CSF3R) (M59820) are found to be upregulated and would thus be considered targets for downregulation in MS. In contrast, the 5-HT6 serotonin receptor (L41147), and the STAT2 transcription factor (U18671) are downregulated, and therefore we propose that attempts to upregulate these transcripts will benefit MS patients. Similar examples of target selection can be extracted from Tables 2-10.

[0046] In Table 2, examples of target genes that are upregulated in MS spinal cords include the inflammation related genes Anti-hepatitis A IgG (*M87789) and the metal ion-related NRAMP1 (D50402). Downregulated genes that could be targeted for treating MS include the neurofilament triplet protein L (U57341), involved in neuronal cytoskeletal integrity, and a lymphoid specific transcription factor (M36542).

[0047] In Table 3, examples of target genes that are upregulated in MS spinal cords include the inflammation related genes CD14 (*X13334), C5a anaphylatoxin receptor (M62505), Fc receptor Iib3 for IgG (Affymetrix designation HG491-HT491), lymph node homing receptor (M25280), and the complement component properdin (M83652). Also in Table 3, downregulated genes that could be used as targets of treatment include guanylate kinase (L76200) involved in DNA repair, and mitochondrial creatine kinase (J04469) involved in energy metabolism.

[0048] In Table 4, elevated transcripts for the inflammation-related genes cathepsin C (X87212), T cell receptor zeta chain (J04132), and MHC class II HLA (M96132) may serve as targets of treatment. From Table 5, elevated phospholipid transfer protein (HG3945-HT4215), and downregulated transcripts for the DNA mismatch repair gene MLH1 (AF001359) and the glutamate transporter EAAT3 (U08989) are candidate targets. From Table 6, the downregulated TGF-beta superfamily protein (AB000584) may be used as a example. From Table 7, the repair gene Rad23A homolog (AD000092) was also downregulated. From Table 8, the apoptosis-related phospholipid scramblase (AF008445) is found to be an elevated target transcript. From Table 9, the inhibitor of apoptosis protein 1 (U45878) is downregulated, and elevation of its expression could prevent (neuronal) cell death. The immune attenuator CD152/CTLA4 (Y10514) is also downregulated, and elevation of its expression could attenuate inflammation in MS. The checkpoint suppressor 1 (U68723) is also found to be elevated. From Table 10, upregulated transcripts that are hereby proposed as targets of MS treatments include acid ceramidase (U70063), the MHC-binding protein 2 MBP2 (X65644), and choline kinase (*D10704). Also, from Table 11, decreased mitochondrial ATP synthase (X69908), and increased interferon γ (IFN-γ) receptor a chain (U19247) can be used as targets of treatment. A similar approach can be implemented for selecting genes from Tables 12 to 15.

[0049] The above genes are mentioned only by way of example, for a concept of treating MS that can be applied to all other genes in the list. Various aspects of gene delivery and expression are set forth below.

[0050] 1. Therapeutic Transgenes

[0051] Thus, in accordance with the present invention, there are provided methods of treating and preventing MS utilizing genes identified as being overexpressed or underexpressed in MS, as illustrated in Tables 1-15. By inhibiting or increasing the expression of various of these genes, therapeutic benefit may be provided to patients.

[0052] 2. Antisense

[0053] In contrast to “replacement” gene therapy, described above, it may be desirable to down-regulate the expression of certain targets that are overexpressed in individuals afflicted with, or at risk of, MS. A variety of mechanisms are available for effecting a decrease in gene expression using genetic constructs.

[0054] The term “antisense” nucleic acid refers to oligo- and polynucleotides complementary to bases sequences of a target DNA or RNA. When introduced into a cell, antisense molecules hybridize to a target nucleic acid and interfere with its transcription, transport, processing, splicing or translation. Targeting double-stranded DNA leads to triple helix formation; targeting RNA will lead to double helix formation.

[0055] Antisense constructs may be designed to bind to the promoter or other control regions, exons, introns or even exon-intron boundaries of a gene. Antisense RNA constructs, or DNA encoding such antisense RNA's, may be employed to inhibit gene transcription or translation within a host cell. Nucleic acid sequences which comprise “complementary nucleotides” are those which are capable of base-pairing according to the standard Watson-Crick complementarity rules. That is, that the larger purines will base pair with the smaller pyrimidines to form combinations of guanine paired with cytosine (G:C) and adenine paired with either thymine in the case of DNA (A:T), or uracil (A:U) in the case of RNA. Inclusion of less common bases such as inosine, 5-methylcytosine, 6-methyladenine, hypoxanthine and others in hybridizing sequences does not interfere with pairing.

[0056] As used herein, the terms “complementary” and “antisense sequences” mean nucleic acid sequences that are substantially complementary over their entire length and have very few base mismatches. For example, nucleic acid sequences of fifteen bases in length may be termed complementary when they have complementary nucleotides at thirteen or fourteen positions. Naturally, nucleic acid sequences which are “completely complementary” will be nucleic acid sequences which have perfect base pair matching with the target sequences, i.e., no mismatches. Other sequences with lower degrees of homology are contemplated. For example, an antisense construct with limited regions of high homology, but overall containing a lower degree (50% or less) total homology, may be used.

[0057] While all or part of the gene sequence may be employed in the context of antisense construction, statistically, any sequence of 17 bases long should occur only once in the human genome and, therefore, suffice to specify a unique target. Although shorter oligomers are easier to make and increase in vivo accessibility, numerous other factors are involved in determining the specificity of hybridization. Both binding affinity and sequence specificity of an oligonucleotide to its complementary target increases with increasing length. It is contemplated that oligonucleotides of 8, 9, 10, 11, 12, 13, 14, 15, 16, 17, 18, 19, 20 or more base pairs will be used. One can readily determine whether a given antisense nucleic acid is effective at targeting a gene simply by testing the construct in vitro to determine whether the gene's function or expression is affected.

[0058] In certain embodiments, one may wish to employ antisense constructs which include other elements, for example, those which include C-5 propyne pyrimidines. Oligonucleotides which contain C-5 propyne analogs of uridine and cytidine have been shown to bind RNA with high affinity and to be potent inhibitors or gene expression. Wagner et al. (1993).

[0059] 3. Ribozymes

[0060] The term “ribozyme” refers to an RNA-based enzyme capable of targeting and cleaving particular DNA and RNA sequences. Ribozymes can either be targeted directly to cells, in the form of RNA oligonucleotides incorporating ribozyme sequences, or introduced into the cell as an expression construct encoding the desired ribozymal RNA. Ribozymes may be used and applied in much the same way as described for antisense nucleic acids. Ribozyme sequences also may be modified in much the same way as described for antisense nucleic acids. For example, one could include modified bases or modified phosphate backbones to improve stability or function.

[0061] 4. RNA Interference

[0062] RNA interference (RNAi) is a form of gene silencing triggered by double-stranded RNA (dsRNA). DsRNA activates post-transcriptional gene expression surveillance mechanisms that appear to function to defend cells from virus infection and transposon activity. Fire et al. (1998); Grishok et al. (2000); Ketting et al. (1999); Lin & Avery (1999); Montgomery et al. (1998); Sharp (1999); Sharp & Zamore (2000); Tabara et al. (1999). Activation of these mechanisms targets mature, dsRNA-complementary mRNA for destruction. RNA_(i) offers major experimental advantages for study of gene function. These advantages include a very high specificity, ease of movement across cell membranes, and prolonged down-regulation of the targeted gene. Fire et al. (1998); Grishok et al. (2000); Ketting et al. (1999); Lin & Avery (1999); Montgomery et al. (1998); Sharp (1999); Sharp & Zamore (2000); Tabara et al. (1999). Moreover, dsRNA has been shown to silence genes in a wide range of systems, including plants, protozoans, fungi, C. elegans, Trypanosoma and Drosophila. Grishok et al. (2000); Sharp (1999); Sharp & Zamore (1999).

[0063] Several principles are worth note (see Plasterk & Ketting, 2000) First, the dsRNA should be directed to an exon, although some exceptions to this rule have been shown. Second, a homology threshold (probably about 80-85% over 200 bases) is required. Most tested sequences are 500 base pairs or greater. Third, the targeted mRNA is lost after RNA_(i). Fourth, the effect is non-stoichometric, and thus incredibly potent. In fact, it has been estimated that only a few copies of dsRNA are required to knock down >95% of targeted gene expression in a cell. Fire et al. (1998). Recently, shorter (˜20 base pairs) synthetic duplex RNAs have been shown to efficiently perform RNAi, by using liposome transfection. Further, similar short interfering RNA (siRNA) duplexes of 19-25 base pairs have been used by transfection via recombinant DNA constructs containing a promoter for U6 small nuclear RNA (snRNA) to drive nuclear expression of a single RNA transcript. This is also known as the hairpin siRNA/suppression of endogenous RNA (SUPER) strategy and has been shown to eliminate the expression of a target gene in long-term mammalian cell cultures (Brummelkamp et al., 2002; Paul et al., 2002; Lee et al., 2002; Miyagishi et al., 2002).

[0064] Although the precise mechanism of RNA_(i) is still unknown, the involvement of permanent gene modification or the disruption of transcription have been experimentally eliminated. It is now generally accepted that RNA_(i) acts post-transcriptionally, targeting RNA transcripts for degradation. It appears that both nuclear and cytoplasmic RNA can be targeted. Bosher and Labouesse (2000).

[0065] 5. Single Chain Antibodies

[0066] Naturally-occurring antibodies (of isotype IgG) produced by B cells, consist of four polypeptide chains. Two heavy chains (composed of four immunoglobulin domains) and two light chains (made up of two immunoglobulin domains) are held together by disulphide bonds. The bulk of the antibody complex is made up of constant immunoglobulin domains. These have a conserved amino acid sequence, and exhibit low variability. Different classes of constant regions in the stem of the antibody generate different isotypes of antibody with differing properties. The recognition properties of the antibody are carried by the variable regions (VH and VL) at the ends of the arms. Each variable domain contains three hypervariable regions known as complementarity determining regions, or CDRs. The CDRs come together in the final tertiary structure to form an antigen binding pocket. The human genome contains multiple fragments encoding portions of the variable domains in regions of the immunoglobulin gene cluster known as V, D and J. During B cell development these regions undergo recombination to generate a broad diversity of antibody affinities. As these B cell populations mature in the presence of a target antigen, hypermutation of the variable region takes place, with the B cells producing the most active antibodies being selected for further expansion in a process known as affinity maturation.

[0067] A major breakthrough was the generation of monoclonal antibodies, pure populations of antibodies with the same affinity. This was achieved by fusing B cells taken from immunized animals with myeloma cells. This generates a population of immortal hybridomas, from which the required clones can be selected. Monoclonal antibodies are very important research tools, and have been used in some therapies. However, they are very expensive and difficult to produce, and if used in a therapeutic context, can elicit and immune response which will destroy the antibody. This can be reduced in part by humanizing the antibody by grafting the CDRs from the parent monoclonal into the backbone of a human IgG antibody. It may be better to deliver antibodies by gene therapy, as this would hopefully provide a constant localized supply of antibody following a single dose of vector. The problems of vector design and delivery are dealt with elsewhere, but antibodies in their native form, consisting of two different polypeptide chains which need to be generated in approximately equal amounts and assembled correctly are not good candidates for gene therapy. However, it is possible to create a single polypeptide which can retain the antigen binding properties of a monoclonal antibody.

[0068] The variable regions from the heavy and light chains (VH and VL) are both approximately 110 amino acids long. They can be linked by a 15 amino acid linker (e.g., (glycine₄serine)₃), which has sufficient flexibility to allow the two domains to assemble a functional antigen binding pocket. Addition of various signal sequences allows the scFv to be targeted to different organelles within the cell, or to be secreted. Addition of the light chain constant region (Ck) allows dimerization via disulphide bonds, giving increased stability and avidity. However, there is evidence that scFvs spontaneously multimerize, with the extent of aggregation (presumably via exposed hydrophobic surfaces) being dependent on the length of the glycine-serine linker.

[0069] The variable regions for constructing the scFv are obtained as follows. Using a monoclonal antibody against the target of interest, it is a simple procedure to use RT-PCR to clone out the variable regions from mRNA extracted from the parent hybridoma. Degenerate primers targeted to the relatively invariant framework regions can be used. Expression constructs are available with convenient cloning sites for the insertion of the cloned variable regions.

[0070] 6. Vectors

[0071] In accordance with the present invention, both stimulatory and inhibitory genes may be provided to cells of an MS patient and expressed therein. Stimulatory genes are generally simply copies of the gene of interest, although in some cases they may be genes, the expression of which direct the expression of the gene of interest. Inhibitory genes, discussed above, may include antisense or single-chain antibody genes.

[0072] The term “vector” is used to refer to a carrier nucleic acid molecule into which a nucleic acid sequence can be inserted for introduction into a cell where it can be replicated. A nucleic acid sequence can be “exogenous,” which means that it is foreign to the cell into which the vector is being introduced or that the sequence is homologous to a sequence in the cell but in a position within the host cell nucleic acid in which the sequence is ordinarily not found. Vectors include plasmids, cosmids, viruses (bacteriophage, animal viruses, and plant viruses), and artificial chromosomes (e.g., YACs). One of skill in the art would be well equipped to construct a vector through standard recombinant techniques (see, for example, Maniatis et al., 1989 and Ausubel et al., 1994, both incorporated herein by reference).

[0073] The term “expression vector” refers to any type of genetic construct comprising a nucleic acid coding for a RNA capable of being transcribed. In some cases, RNA molecules are then translated into a protein, polypeptide, or peptide. In other cases, these sequences are not translated, for example, in the production of antisense molecules or ribozymes. Expression vectors can contain a variety of “control sequences,” which refer to nucleic acid sequences necessary for the transcription and possibly translation of an operably linked coding sequence in a particular host cell. In addition to control sequences that govern transcription and translation, vectors and expression vectors may contain nucleic acid sequences that serve other functions as well and are described infra.

[0074] a. Promoters and Enhancers

[0075] A “promoter” is a control sequence that is a region of a nucleic acid sequence at which initiation and rate of transcription are controlled. It may contain genetic elements at which regulatory proteins and molecules may bind, such as RNA polymerase and other transcription factors, to initiate the specific transcription of a nucleic acid sequence. The phrases “operatively positioned,” “operatively linked,” “under control,” and “under transcriptional control” mean that a promoter is in a correct functional location and/or orientation in relation to a nucleic acid sequence to control transcriptional initiation and/or expression of that sequence.

[0076] A promoter generally comprises a sequence that functions to position the start site for RNA synthesis. The best known example of this is the TATA box, but in some promoters lacking a TATA box, such as, for example, the promoter for the mammalian terminal deoxynucleotidyl transferase gene and the promoter for the SV40 late genes, a discrete element overlying the start site itself helps to fix the place of initiation. Additional promoter elements regulate the frequency of transcriptional initiation. Typically, these are located in the region 30-110 bp upstream of the start site, although a number of promoters have been shown to contain functional elements downstream of the start site as well. To bring a coding sequence “under the control of” promoter, one positions the 5′ end of the transcription initiation site of the transcriptional reading frame “downstream” of (i.e., 3′ of) the chosen promoter. The “upstream” promoter stimulates transcription of the DNA and promotes expression of the encoded RNA.

[0077] The spacing between promoter elements frequently is flexible, so that promoter function is preserved when elements are inverted or moved relative to one another. In the tk promoter, the spacing between promoter elements can be increased to 50 bp apart before activity begins to decline. Depending on the promoter, it appears that individual elements can function either cooperatively or independently to activate transcription. A promoter may or may not be used in conjunction with an “enhancer,” which refers to a cis-acting regulatory sequence involved in the transcriptional activation of a nucleic acid sequence.

[0078] A promoter may be one naturally associated with a nucleic acid sequence, as may be obtained by isolating the 5′ non-coding sequences located upstream of the coding segment and/or exon. Such a promoter can be referred to as “endogenous.” Similarly, an enhancer may be one naturally associated with a nucleic acid sequence, located either downstream or upstream of that sequence. Alternatively, certain advantages will be gained by positioning the coding nucleic acid segment under the control of a recombinant or heterologous promoter, which refers to a promoter that is not normally associated with a nucleic acid sequence in its natural environment. A recombinant or heterologous enhancer refers also to an enhancer not normally associated with a nucleic acid sequence in its natural environment. Such promoters or enhancers may include promoters or enhancers of other genes, and promoters or enhancers isolated from any other virus, or prokaryotic or eukaryotic cell, and promoters or enhancers not “naturally occurring,” i.e., containing different elements of different transcriptional regulatory regions, and/or mutations that alter expression. For example, promoters that are most commonly used in recombinant DNA construction include the β-lactamase (penicillinase), lactose and tryptophan (trp) promoter systems. In addition to producing nucleic acid sequences of promoters and enhancers synthetically, sequences may be produced using recombinant cloning and/or nucleic acid amplification technology, including PCR™, in connection with the compositions disclosed herein (see U.S. Pat. Nos. 4,683,202 and 5,928,906, each incorporated herein by reference). Furthermore, it is contemplated the control sequences that direct transcription and/or expression of sequences within non-nuclear organelles such as mitochondria, chloroplasts, and the like, can be employed as well.

[0079] Naturally, it will be important to employ a promoter and/or enhancer that effectively directs the expression of the DNA segment in the organelle, cell type, tissue, organ, or organism chosen for expression. Those of skill in the art of molecular biology generally know the use of promoters, enhancers, and cell type combinations for protein expression, (see, for example Sambrook et al. 1989, incorporated herein by reference). The promoters employed may be constitutive, tissue-specific, inducible, and/or useful under the appropriate conditions to direct high level expression of the introduced DNA segment, such as is advantageous in the large-scale production of recombinant proteins and/or peptides. The promoter may be heterologous or endogenous.

[0080] Additionally any promoter/enhancer combination (as per, for example, the Eukaryotic Promoter Data Base EPDB, www.epd.isb-sib.ch/) could also be used to drive expression. Use of a T3, T7 or SP6 cytoplasmic expression system is another possible embodiment. Eukaryotic cells can support cytoplasmic transcription from certain bacterial promoters if the appropriate bacterial polymerase is provided, either as part of the delivery complex or as an additional genetic expression construct.

[0081] Table 19 lists non-limiting examples of elements/promoters that may be employed, in the context of the present invention, to regulate the expression of a RNA. Table 20 provides non-limiting examples of inducible elements, which are regions of a nucleic acid sequence that can be activated in response to a specific stimulus. TABLE 19 Promoter and/or Enhancer Promoter/Enhancer References Immunoglobulin Heavy Chain Banerji et al., 1983; Gilles et al., 1983; Grosschedl et al., 1985; Atchinson et al., 1986, 1987; Imler et al., 1987; Weinberger et al., 1984; Kiledjian et al., 1988; Porton et al.; 1990 Immunoglobulin Light Chain Queen et al., 1983; Picard et al., 1984 T-Cell Receptor Luria et al., 1987; Winoto et al., 1989; Redondo et al.; 1990 HLA DQ a and/or DQ β Sullivan et al., 1987 β-Interferon Goodbourn et al., 1986; Fujita et al., 1987; Goodbourn et al., 1988 Interleukin-2 Greene et al., 1989 Interleukin-2 Receptor Greene et al., 1989; Lin et al., 1990 MHC Class II 5 Koch et al., 1989 MHC Class II HLA-Dra Sherman et al., 1989 β-Actin Kawamoto et al., 1988; Ng et al.; 1989 Muscle Creatine Kinase (MCK) Jaynes et al., 1988; Horlick et al., 1989; Johnson et al., 1989 Prealbumin (Transthyretin) Costa et al., 1988 Elastase I Ornitz et al., 1987 Metallothionein (MTII) Karin et al., 1987; Culotta et al., 1989 Collagenase Pinkert et al., 1987; Angel et al., 1987 Albumin Pinkert et al., 1987; Tronche et al., 1989, 1990 α-Fetoprotein Godbout et al., 1988; Campere et al., 1989 γ-Globin Bodine et al., 1987; Perez-Stable et al., 1990 β-Globin Trudel et al., 1987 c-fos Cohen et al., 1987 c-HA-ras Triesman, 1986; Deschamps et al., 1985 Insulin Edlund et al., 1985 Neural Cell Adhesion Molecule Hirsch et al., 1990 (NCAM) α₁-Antitrypsin Latimer et al., 1990 H2B (TH2B) Histone Hwang et al., 1990 Mouse and/or Type I Collagen Ripe et al., 1989 Glucose-Regulated Proteins Chang et al., 1989 (GRP94 and GRP78) Rat Growth Hormone Larsen et al., 1986 Human Serum Amyloid A (SAA) Edbrooke et al., 1989 Troponin I (TN I) Yutzey et al., 1989 Platelet-Derived Growth Factor Pech et al., 1989 (PDGF) Duchenne Muscular Dystrophy Klamut et al., 1990 SV40 Banerji et al., 1981; Moreau et al., 1981; Sleigh et al., 1985; Firak et al., 1986; Herr et al., 1986; Imbra et al., 1986; Kadesch et al., 1986; Wang et al., 1986; Ondek et al., 1987; Kuhl et al., 1987; Schaffner et al., 1988 Polyoma Swartzendruber et al., 1975; Vasseur et al., 1980; Katinka et al., 1980, 1981; Tyndell et al., 1981; Dandolo et al., 1983; de Villiers et al., 1984; Hen et al., 1986; Satake et al., 1988; Campbell and/or Villarreal, 1988 Retroviruses Kriegler et al., 1982, 1983; Levinson et al., 1982; Kriegler et al., 1983, 1984a, b, 1988; Bosze et al., 1986; Miksicek et al., 1986; Celander et al., 1987; Thiesen et al., 1988; Celander et al., 1988; Choi et al., 1988; Reisman et al., 1989 Papilloma Virus Campo et al., 1983; Lusky et al., 1983; Spandidos and/or Wilkie, 1983; Spalholz et al., 1985; Lusky et al., 1986; Cripe et al., 1987; Gloss et al., 1987; Hirochika et al., 1987; Stephens et al., 1987 Hepatitis B Virus Bulla et al., 1986; Jameel et al., 1986; Shaul et al., 1987; Spandau et al., 1988; Vannice et al., 1988 Human Immunodeficiency Virus Muesing et al., 1987; Hauber et al., 1988; Jakobovits et al., 1988; Feng et al., 1988; Takebe et al., 1988; Rosen et al., 1988; Berkhout et al., 1989; Laspia et al., 1989; Sharp et al., 1989; Braddock et al., 1989 Cytomegalovirus (CMV) Weber et al., 1984; Boshart et al., 1985; Foecking et al., 1986 Gibbon Ape Leukemia Virus Holbrook et al., 1987; Quinn et al., 1989

[0082] TABLE 20 Inducible Elements Element Inducer References MT II Phorbol Ester (TFA) Palmiter et al., 1982; Haslinger et Heavy metals al., 1985; Searle et al., 1985; Stuart et al., 1985; Imagawa et al., 1987, Karin et al., 1987; Angel et al., 1987b; McNeall et al., 1989 MMTV (mouse mammary Glucocorticoids Huang et al., 1981; Lee et al., tumor virus) 1981; Majors et al., 1983; Chandler et al., 1983; Lee et al., 1984; Ponta et al., 1985; Sakai et al., 1988 β-Interferon Poly(rI)x Tavernier et al., 1983 Poly(rc) Adenovirus 5 E2 ElA Imperiale et al., 1984 Collagenase Phorbol Ester (TPA) Angel et al., 1987a Stromelysin Phorbol Ester (TPA) Angel et al., 1987b SV40 Phorbol Ester (TPA) Angel et al., 1987b Murine MX Gene Interferon, Newcastle Hug et al., 1988 Disease Virus GRP78 Gene A23187 Resendez et al., 1988 α-2-Macroglobulin IL-6 Kunz et al., 1989 Vimentin Serum Rittling et al., 1989 MHC Class I Gene H-2κb Interferon Blanar et al., 1989 HSP70 ElA, SV40 Large T Taylor et al., 1989, 1990a, 1990b Antigen Proliferin Phorbol Ester-TPA Mordacq et al., 1989 Tumor Necrosis Factor α PMA Hensel et al., 1989 Thyroid Stimulating Thyroid Hormone Chatterjee et al., 1989 Hormone α Gene

[0083] The identity of tissue-specific promoters or elements, as well as assays to characterize their activity, is well known to those of skill in the art. Non-limiting examples of such regions include the human LIMK2 gene (Nomoto et al., 1999), the somatostatin receptor 2 gene (Kraus et al., 1998), murine epididymal retinoic acid-binding gene (Lareyre et al., 1999), human CD4 (Zhao-Emonet et al., 1998), mouse α2 (XI) collagen (Tsumaki et al., 1998), D1A dopamine receptor gene (Lee et al., 1997), insulin-like growth factor II (Wu et al., 1997), and human platelet endothelial cell adhesion molecule-1 (Almendro et al., 1996). Of particular interest are the neuronal promoter NSE (neuron-specific enolase), and the glial promoter GFAP (glial fibrillary acidic protein).

[0084] b. Initiation Signals and Internal Ribosome Binding Sites

[0085] A specific initiation signal also may be required for efficient translation of coding sequences. These signals include the ATG initiation codon or adjacent sequences. Exogenous translational control signals, including the ATG initiation codon, may need to be provided. One of ordinary skill in the art would readily be capable of determining this and providing the necessary signals. It is well known that the initiation codon must be “in-frame” with the reading frame of the desired coding sequence to ensure translation of the entire insert. The exogenous translational control signals and initiation codons can be either natural or synthetic. The efficiency of expression may be enhanced by the inclusion of appropriate transcription enhancer elements.

[0086] In certain embodiments of the invention, the use of internal ribosome entry sites (IRES) elements are used to create multigene, or polycistronic, messages. IRES elements are able to bypass the ribosome scanning model of 5′-methylated Cap dependent translation and begin translation at internal sites (Pelletier and Sonenberg, 1988). IRES elements from two members of the picornavirus family (polio and encephalomyocarditis) have been described (Pelletier and Sonenberg, 1988), as well an IRES from a mammalian message (Macejak and Samow, 1991). IRES elements can be linked to heterologous open reading frames. Multiple open reading frames can be transcribed together, each separated by an IRES, creating polycistronic messages. By virtue of the IRES element, each open reading frame is accessible to ribosomes for efficient translation. Multiple genes can be efficiently expressed using a single promoter/enhancer to transcribe a single message (see U.S. Pat. Nos. 5,925,565 and 5,935,819, each herein incorporated by reference).

[0087] c. Multiple Cloning Sites

[0088] Vectors can include a multiple cloning site (MCS), which is a nucleic acid region that contains multiple restriction enzyme sites, any of which can be used in conjunction with standard recombinant technology to digest the vector (see, for example, Carbonelli et al., 1999, Levenson et al., 1998, and Cocea, 1997, incorporated herein by reference.) “Restriction enzyme digestion” refers to catalytic cleavage of a nucleic acid molecule with an enzyme that functions only at specific locations in a nucleic acid molecule. Many of these restriction enzymes are commercially available. Use of such enzymes is widely understood by those of skill in the art. Frequently, a vector is linearized or fragmented using a restriction enzyme that cuts within the MCS to enable exogenous sequences to be ligated to the vector. “Ligation” refers to the process of forming phosphodiester bonds between two nucleic acid fragments, which may or may not be contiguous with each other. Techniques involving restriction enzymes and ligation reactions are well known to those of skill in the art of recombinant technology.

[0089] d. Splicing Sites

[0090] Most transcribed eukaryotic RNA molecules will undergo RNA splicing to remove introns from the primary transcripts. Vectors containing genomic eukaryotic sequences may require donor and/or acceptor splicing sites to ensure proper processing of the transcript for protein expression (see, for example, Chandler et al., 1997, herein incorporated by reference).

[0091] e. Termination Signals

[0092] The vectors or constructs of the present invention will generally comprise at least one termination signal. A “termination signal” or “terminator” is comprised of the DNA sequences involved in specific termination of an RNA transcript by an RNA polymerase. Thus, in certain embodiments a termination signal that ends the production of an RNA transcript is contemplated.

[0093] A terminator may be necessary in vivo to achieve desirable message levels. In eukaryotic systems, the terminator region may also comprise specific DNA sequences that permit site-specific cleavage of the new transcript so as to expose a polyadenylation site. This signals a specialized endogenous polymerase to add a stretch of about 200 A residues (polyA) to the 3′ end of the transcript. RNA molecules modified with this polyA tail appear to more stable and are translated more efficiently. Thus, in other embodiments involving eukaryotes, it is preferred that that terminator comprises a signal for the cleavage of the RNA, and it is more preferred that the terminator signal promotes polyadenylation of the message. The terminator and/or polyadenylation site elements can serve to enhance message levels and to minimize read through from the cassette into other sequences.

[0094] Terminators contemplated for use in the invention include any known terminator of transcription described herein or known to one of ordinary skill in the art, including but not limited to, for example, the termination sequences of genes, such as for example the bovine growth hormone terminator or viral termination sequences, such as for example the SV40 terminator. In certain embodiments, the termination signal may be a lack of transcribable or translatable sequence, such as due to a sequence truncation.

[0095] f. Polyadenylation Signals

[0096] In expression, particularly eukaryotic expression, one will typically include a polyadenylation signal to effect proper polyadenylation of the transcript. The nature of the polyadenylation signal is not believed to be crucial to the successful practice of the invention, and any such sequence may be employed. Preferred embodiments include the SV40 polyadenylation signal or the bovine growth hormone polyadenylation signal, convenient and known to function well in various target cells. Polyadenylation may increase the stability of the transcript or may facilitate cytoplasmic transport.

[0097] g. Origins of Replication

[0098] In order to propagate a vector in a host cell, it may contain one or more origins of replication sites (often termed “ori”), which is a specific nucleic acid sequence at which replication is initiated. Alternatively an autonomously replicating sequence (ARS) can be employed if the host cell is yeast.

[0099] h. Selectable and Screenable Markers

[0100] In certain embodiments of the invention, cells containing a nucleic acid construct of the present invention may be identified in vitro or in vivo by including a marker in the expression vector. Such markers would confer an identifiable change to the cell permitting easy identification of cells containing the expression vector. Generally, a selectable marker is one that confers a property that allows for selection. A positive selectable marker is one in which the presence of the marker allows for its selection, while a negative selectable marker is one in which its presence prevents its selection. An example of a positive selectable marker is a drug resistance marker.

[0101] Usually the inclusion of a drug selection marker aids in the cloning and identification of transformants, for example, genes that confer resistance to neomycin, puromycin, hygromycin, DHFR, GPT, zeocin and histidinol are useful selectable markers. In addition to markers conferring a phenotype that allows for the discrimination of transformants based on the implementation of conditions, other types of markers including screenable markers such as GFP, whose basis is calorimetric analysis, are also contemplated. Alternatively, screenable enzymes such as herpes simplex virus thymidine kinase (tk) or chloramphenicol acetyltransferase (CAT) may be utilized. One of skill in the art would also know how to employ immunologic markers, possibly in conjunction with FACS analysis. The marker used is not believed to be important, so long as it is capable of being expressed simultaneously with the nucleic acid encoding a gene product. Further examples of selectable and screenable markers are well known to one of skill in the art.

[0102] i. Plasmid Vectors

[0103] In certain embodiments, a plasmid vector is contemplated for use to transform a host cell. In general, plasmid vectors containing replicon and control sequences which are derived from species compatible with the host cell are used in connection with these hosts. The vector ordinarily carries a replication site, as well as marking sequences which are capable of providing phenotypic selection in transformed cells. In a non-limiting example, E. coli is often transformed using derivatives of pBR322, a plasmid derived from an E. coli species. pBR322 contains genes for ampicillin and tetracycline resistance and thus provides easy means for identifying transformed cells. The pBR plasmid, or other microbial plasmid or phage must also contain, or be modified to contain, for example, promoters which can be used by the microbial organism for expression of its own proteins.

[0104] In addition, phage vectors containing replicon and control sequences that are compatible with the host microorganism can be used as transforming vectors in connection with these hosts. For example, the phage lambda GEM™-11 may be utilized in making a recombinant phage vector which can be used to transform host cells, such as, for example, E. coli LE392. Further useful plasmid vectors include pIN vectors (Inouye et al., 1985); and pGEX vectors, for use in generating glutathione S-transferase (GST) soluble fusion proteins for later purification and separation or cleavage. Other suitable fusion proteins are those with β-galactosidase, ubiquitin, and the like.

[0105] Bacterial host cells, for example, E. coli, comprising the expression vector, are grown in any of a number of suitable media, for example, LB. The expression of the recombinant protein in certain vectors may be induced, as would be understood by those of skill in the art, by contacting a host cell with an agent specific for certain promoters, e.g., by adding IPTG to the media or by switching incubation to a higher temperature. After culturing the bacteria for a further period, generally of between 2 and 24 h, the cells are collected by centrifugation and washed to remove residual media.

[0106] j. Viral Vectors

[0107] The ability of certain viruses to infect cells or enter cells via receptor-mediated endocytosis, and to integrate into host cell genome and express viral genes stably and efficiently have made them attractive candidates for the transfer of foreign nucleic acids into cells (e.g., mammalian cells). Non-limiting examples of virus vectors that may be used to deliver a nucleic acid of the present invention are described below.

[0108] 1. Adenoviral Vectors

[0109] A particular method for delivery of the nucleic acid involves the use of an adenovirus expression vector. Although adenovirus vectors are known to have a low capacity for integration into genomic DNA, this feature is counterbalanced by the high efficiency of gene transfer afforded by these vectors. “Adenovirus expression vector” is meant to include those constructs containing adenovirus sequences sufficient to (a) support packaging of the construct and (b) to ultimately express a tissue or cell-specific construct that has been cloned therein. Knowledge of the genetic organization or adenovirus, a 36 kb, linear, double-stranded DNA virus, allows substitution of large pieces of adenoviral DNA with foreign sequences up to 7 kb (Grunhaus and Horwitz, 1992).

[0110] 2. AAV Vectors

[0111] The nucleic acid may be introduced into the cell using adenovirus assisted transfection. Increased transfection efficiencies have been reported in cell systems using adenovirus coupled systems (Kelleher and Vos, 1994; Cotten et al., 1992; Curiel, 1994). Adeno-associated virus (AAV) is an attractive vector system as it has a high frequency of integration and it can infect non-dividing cells, thus making it useful for delivery of genes into mammalian cells, for example, in tissue culture (Muzyczka, 1992) or in vivo. AAV has a broad host range for infectivity (Tratschin et al., 1984; Laughlin et al., 1986; Lebkowski et al., 1988; McLaughlin et al., 1988). Details concerning the generation and use of rAAV vectors are described in U.S. Pat. Nos. 5,139,941 and 4,797,368, each incorporated herein by reference.

[0112] 3. Retroviral Vectors

[0113] Retroviruses have promise as gene delivery vectors due to their ability to integrate their genes into the host genome, transferring a large amount of foreign genetic material, infecting a broad spectrum of species and cell types and of being packaged in special cell-lines (Miller, 1992).

[0114] In order to construct a retroviral vector, a nucleic acid (e.g., one encoding gene of interest) is inserted into the viral genome in the place of certain viral sequences to produce a virus that is replication-defective. In order to produce virions, a packaging cell line containing the gag, pol, and env genes but without the LTR and packaging components is constructed (Mann et al., 1983). When a recombinant plasmid containing a cDNA, together with the retroviral LTR and packaging sequences is introduced into a special cell line (e.g., by calcium phosphate precipitation for example), the packaging sequence allows the RNA transcript of the recombinant plasmid to be packaged into viral particles, which are then secreted into the culture media (Nicolas and Rubenstein, 1988; Temin, 1986; Mann et al., 1983). The media containing the recombinant retroviruses is then collected, optionally concentrated, and used for gene transfer. Retroviral vectors are able to infect a broad variety of cell types. However, integration and stable expression require the division of host cells (Paskind et al., 1975).

[0115] Lentiviruses are complex retroviruses, which, in addition to the common retroviral genes gag, pol, and env, contain other genes with regulatory or structural function. Lentiviral vectors are well known in the art (see, for example, Naldini et al., 1996; Zufferey et al., 1997; Blomer et al., 1997; U.S. Pat. Nos. 6,013,516 and 5,994,136). Some examples of lentivirus include the Human Immunodeficiency Viruses: HIV-1, HIV-2 and the Simian Immunodeficiency Virus: SIV. Lentiviral vectors have been generated by multiply attenuating the HIV virulence genes, for example, the genes env, vif, vpr, vpu and nef are deleted making the vector biologically safe. Recombinant lentiviral vectors are capable of infecting non-dividing cells and can be used for both in vivo and ex vivo gene transfer and expression of nucleic acid sequences. For example, recombinant lentivirus capable of infecting a non-dividing cell wherein a suitable host cell is transfected with two or more vectors carrying the packaging functions, namely gag, pol and env, as well as rev and tat is described in U.S. Pat. No. 5,994,136, incorporated herein by reference. One may target the recombinant virus by linkage of the envelope protein with an antibody or a particular ligand for targeting to a receptor of a particular cell-type. By inserting a sequence (including a regulatory region) of interest into the viral vector, along with another gene which encodes the ligand for a receptor on a specific target cell, for example, the vector is now target-specific.

[0116] 4. Other Viral Vectors

[0117] Other viral vectors may be employed as vaccine constructs in the present invention. Vectors derived from viruses such as vaccinia virus (Ridgeway, 1988; Baichwal and Sugden, 1986; Coupar et al., 1988), sindbis virus, cytomegalovirus and herpes simplex virus may be employed. They offer several attractive features for various mammalian cells (Friedmann, 1989; Ridgeway, 1988; Baichwal and Sugden, 1986; Coupar et al., 1988; Horwich et al., 1990).

[0118] 5. Delivery Using Modified Viruses

[0119] A nucleic acid to be delivered may be housed within an infective virus that has been engineered to express a specific binding ligand. The virus particle will thus bind specifically to the cognate receptors of the target cell and deliver the contents to the cell. A novel approach designed to allow specific targeting of retrovirus vectors was developed based on the chemical modification of a retrovirus by the chemical addition of lactose residues to the viral envelope. This modification can permit the specific infection of hepatocytes via sialoglycoprotein receptors.

[0120] Another approach to targeting of recombinant retroviruses was designed in which biotinylated antibodies against a retroviral envelope protein and against a specific cell receptor were used. The antibodies were coupled via the biotin components by using streptavidin (Roux et al., 1989). Using antibodies against major histocompatibility complex class I and class II antigens, they demonstrated the infection of a variety of human cells that bore those surface antigens with an ecotropic virus in vitro (Roux et al., 1989).

[0121] 7. Vector Delivery and Cell Transformation

[0122] Suitable methods for nucleic acid delivery for transformation of an organelle, a cell, a tissue or an organism for use with the current invention are believed to include virtually any method by which a nucleic acid (e.g., DNA) can be introduced into an organelle, a cell, a tissue or an organism, as described herein or as would be known to one of ordinary skill in the art. Such methods include, but are not limited to, direct delivery of DNA such as by ex vivo transfection (Wilson et al., 1989, Nabel and Baltimore, 1987), by injection (U.S. Pat. Nos. 5,994,624, 5,981,274, 5,945,100, 5,780,448, 5,736,524, 5,702,932, 5,656,610, 5,589,466 and 5,580,859, each incorporated herein by reference), including microinjection (Harlan and Weintraub, 1985; U.S. Pat. No. 5,789,215, incorporated herein by reference); by electroporation (U.S. Pat. No. 5,384,253, incorporated herein by reference; Tur-Kaspa et al., 1986; Potter et al., 1984); by calcium phosphate precipitation (Graham and Van Der Eb, 1973; Chen and Okayama, 1987; Rippe et al., 1990); by using DEAE-dextran followed by polyethylene glycol (Gopal, 1985); by direct sonic loading (Fechheimer et al., 1987); by liposome mediated transfection (Nicolau and Sene, 1982; Fraley et al., 1979; Nicolau et al., 1987; Wong et al., 1980; Kaneda et al., 1989; Kato et al., 1991) and receptor-mediated transfection (Wu and Wu, 1987; Wu and Wu, 1988); by microprojectile bombardment (PCT Application Nos. WO 94/09699 and 95/06128; U.S. Pat. Nos. 5,610,042; 5,322,783 5,563,055, 5,550,318, 5,538,877 and 5,538,880, and each incorporated herein by reference); by agitation with silicon carbide fibers (Kaeppler et al., 1990; U.S. Pat. Nos. 5,302,523 and 5,464,765, each incorporated herein by reference); by PEG-mediated transformation of protoplasts (Omirulleh et al., 1993; U.S. Pat. Nos. 4,684,611 and 4,952,500, each incorporated herein by reference); by desiccation/inhibition-mediated DNA uptake (Potrykus et al., 1985), and any combination of such methods. Through the application of techniques such as these, organelle(s), cell(s), tissue(s) or organism(s) may be stably or transiently transformed.

[0123] a. Injection

[0124] In certain embodiments, a nucleic acid may be delivered to an organelle, a cell, a tissue or an organism via one or more injections (i.e., a needle injection), such as, for example, subcutaneously, intradermally, intramuscularly, intervenously, intraperitoneally, etc. Methods of injection of vaccines are well known to those of ordinary skill in the art (e.g., injection of a composition comprising a saline solution). Further embodiments of the present invention include the introduction of a nucleic acid by direct microinjection. Direct microinjection has been used to introduce nucleic acid constructs into Xenopus oocytes (Harland and Weintraub, 1985).

[0125] b. Electroporation

[0126] In certain embodiments of the present invention, a nucleic acid is introduced into an organelle, a cell, a tissue or an organism via electroporation. Electroporation involves the exposure of a suspension of cells and DNA to a high-voltage electric discharge. In some variants of this method, certain cell wall-degrading enzymes, such as pectin-degrading enzymes, are employed to render the target recipient cells more susceptible to transformation by electroporation than untreated cells (U.S. Pat. No. 5,384,253, incorporated herein by reference). Alternatively, recipient cells can be made more susceptible to transformation by mechanical wounding.

[0127] Transfection of eukaryotic cells using electroporation has been quite successful. Mouse pre-B lymphocytes have been transfected with human kappa-immunoglobulin genes (Potter et al., 1984), and rat hepatocytes have been transfected with the chloramphenicol acetyltransferase gene (Tur-Kaspa et al., 1986) in this manner.

[0128] c. Calcium Phosphate

[0129] In other embodiments of the present invention, a nucleic acid may be introduced to the cells using calcium phosphate precipitation in an ex vivo context. Human KB cells have been transfected with adenovirus 5 DNA (Graham and Van Der Eb, 1973) using this technique. Also in this manner, mouse L(A9), mouse C127, CHO, CV-1, BHK, NIH3T3 and HeLa cells were transfected with a neomycin marker gene (Chen and Okayama, 1987), and rat hepatocytes were transfected with a variety of marker genes (Rippe et al., 1990).

[0130] d. DEAE-Dextran

[0131] In another embodiment, a nucleic acid is delivered into a cell using DEAE-dextran followed by polyethylene glycol. In this manner, reporter plasmids were introduced into mouse myeloma and erythroleukemia cells (Gopal, 1985).

[0132] e. Sonication Loading

[0133] Additional embodiments of the present invention include the introduction of a nucleic acid by direct sonic loading. LTK⁻ fibroblasts have been transfected with the thymidine kinase gene by sonication loading (Fechheimer et al., 1987).

[0134] f. Liposome-Mediated Transfection

[0135] In a further embodiment of the invention, a nucleic acid may be entrapped in a lipid complex such as, for example, a liposome. Liposomes are vesicular structures characterized by a phospholipid bilayer membrane and an inner aqueous medium. Multilamellar liposomes have multiple lipid layers separated by aqueous medium. They form spontaneously when phospholipids are suspended in an excess of aqueous solution. The lipid components undergo self-rearrangement before the formation of closed structures and entrap water and dissolved solutes between the lipid bilayers (Ghosh and Bachhawat, 1991). Also contemplated is a nucleic acid complexed with Lipofectamine (Gibco BRL) or Superfect (Qiagen).

[0136] Liposome-mediated nucleic acid delivery and expression of foreign DNA in vitro has been very successful (Nicolau and Sene, 1982; Fraley et al., 1979; Nicolau et al., 1987). The feasibility of liposome-mediated delivery and expression of foreign DNA in cultured chick embryo, HeLa and hepatoma cells has also been demonstrated (Wong et al., 1980).

[0137] In certain embodiments of the invention, a liposome may be complexed with a hemagglutinating virus (HVJ). This has been shown to facilitate fusion with the cell membrane and promote cell entry of liposome-encapsulated DNA (Kaneda et al., 1989). In other embodiments, a liposome may be complexed or employed in conjunction with nuclear non-histone chromosomal proteins (HMG-1) (Kato et al., 1991). In yet further embodiments, a liposome may be complexed or employed in conjunction with both HVJ and HMG-1. In other embodiments, a delivery vehicle may comprise a ligand and a liposome.

[0138] g. Receptor Mediated Transfection

[0139] Still further, a nucleic acid may be delivered to a target cell via receptor-mediated delivery vehicles. These take advantage of the selective uptake of macromolecules by receptor-mediated endocytosis that will be occurring in a target cell. In view of the cell type-specific distribution of various receptors, this delivery method adds another degree of specificity to the present invention.

[0140] Certain receptor-mediated gene targeting vehicles comprise a cell receptor-specific ligand and a nucleic acid-binding agent. Others comprise a cell receptor-specific ligand to which the nucleic acid to be delivered has been operatively attached. Several ligands have been used for receptor-mediated gene transfer (Wu and Wu, 1987; Wagner et al., 1990; Perales et al., 1994; Myers, EPO 0273085), which establishes the operability of the technique. Specific delivery in the context of another mammalian cell type has been described (Wu and Wu, 1993; incorporated herein by reference). In certain aspects of the present invention, a ligand will be chosen to correspond to a receptor specifically expressed on the target cell population.

[0141] In other embodiments, a nucleic acid delivery vehicle component of a cell-specific nucleic acid targeting vehicle may comprise a specific binding ligand in combination with a liposome. The nucleic acid(s) to be delivered are housed within the liposome and the specific binding ligand is functionally incorporated into the liposome membrane. The liposome will thus specifically bind to the receptor(s) of a target cell and deliver the contents to a cell. Such systems have been shown to be functional using systems in which, for example, epidermal growth factor (EGF) is used in the receptor-mediated delivery of a nucleic acid to cells that exhibit upregulation of the EGF receptor.

[0142] In still further embodiments, the nucleic acid delivery vehicle component of a targeted delivery vehicle may be a liposome itself, which will preferably comprise one or more lipids or glycoproteins that direct cell-specific binding. For example, lactosyl-ceramide, a galactose-terminal asialganglioside, has been incorporated into liposomes and an increase in the uptake of the insulin gene by hepatocytes has been observed (Nicolau et al., 1987). It is contemplated that the tissue-specific transforming constructs of the present invention can be specifically delivered into a target cell in a similar manner.

[0143] h. Microprojectile Bombardment

[0144] Microprojectile bombardment techniques can be used to introduce a nucleic acid ex vivo into at least one, organelle, cell, or tissue (U.S. Pat. Nos. 5,550,318, 5,538,880, 5,610,042, and PCT Application WO 94/09699; each of which is incorporated herein by reference). This method depends on the ability to accelerate DNA-coated microprojectiles to a high velocity allowing them to pierce cell membranes and enter cells without killing them (Klein et al., 1987). There are a wide variety of microprojectile bombardment techniques known in the art, many of which are applicable to the invention.

[0145] In this microprojectile bombardment, one or more particles may be coated with at least one nucleic acid and delivered into cells by a propelling force. Several devices for accelerating small particles have been developed. One such device relies on a high voltage discharge to generate an electrical current, which in turn provides the motive force (Yang et al., 1990). The microprojectiles used have consisted of biologically inert substances such as tungsten or gold particles or beads. Exemplary particles include those comprised of tungsten, platinum, and preferably, gold. It is contemplated that in some instances DNA precipitation onto metal particles would not be necessary for DNA delivery to a recipient cell using microprojectile bombardment. However, it is contemplated that particles may contain DNA rather than be coated with DNA. DNA-coated particles may increase the level of DNA delivery via particle bombardment but are not, in and of themselves, necessary.

[0146] IV. Methods of Assaying for Alterations in Gene Expression

[0147] In accordance with the present invention, methods are provided for assessing the ability of a genetic construct to alter the expression of target genes in patients suffering from or at risk of MS. In each of these assays, the expression of one or more genes, identified in Tables 1-15, will be measured. Genes that play a role in the immune system can be targeted to, and measured from the peripheral blood cells, or alternatively, targeted to, and measured directly from, the inflammatory lesions (i.e., when lesions are biopsied to rule out tumors). Non-immune genes (for instance, genes associated with neurodegeneration or demyelination) can be targeted to, and measured from (if biopsy is done), the brain or spinal cord lesions, regardless of the presence or absence of inflammation. The following is a discussion of various aspects of these methods.

[0148] 1. Hybridization

[0149] There are a variety of ways by which one can assess gene expression. These methods either look at protein or at mRNA levels. Methods looking at mRNAs all fundamentally rely, at a basic level, on nucleic acid hybridization. Hybridization is defined as the ability of a nucleic acid to selectively form duplex molecules with complementary stretches of DNAs and/or RNAs. Depending on the application envisioned, one would employ varying conditions of hybridization to achieve varying degrees of selectivity of the probe or primers for the target sequence.

[0150] Typically, a probe or primer of between 13 and 100 nucleotides, preferably between 17 and 100 nucleotides in length up to 1-2 kilobases or more in length will allow the formation of a duplex molecule that is both stable and selective. Molecules having complementary sequences over contiguous stretches greater than 20 bases in length are generally preferred, to increase stability and selectivity of the hybrid molecules obtained. One will generally prefer to design nucleic acid molecules for hybridization having one or more complementary sequences of 20 to 30 nucleotides, or even longer where desired. Such fragments may be readily prepared, for example, by directly synthesizing the fragment by chemical means or by introducing selected sequences into recombinant vectors for recombinant production.

[0151] For applications requiring high selectivity, one will typically desire to employ relatively high stringency conditions to form the hybrids. For example, relatively low salt and/or high temperature conditions, such as provided by about 0.02 M to about 0.10 M NaCl at temperatures of about 50° C. to about 70° C. Such high stringency conditions tolerate little, if any, mismatch between the probe or primers and the template or target strand and would be particularly suitable for isolating specific genes or for detecting specific mRNA transcripts. It is generally appreciated that conditions can be rendered more stringent by the addition of increasing amounts of formamide.

[0152] For certain applications, for example, lower stringency conditions may be used. Under these conditions, hybridization may occur even though the sequences of the hybridizing strands are not perfectly complementary, but are mismatched at one or more positions. Conditions may be rendered less stringent by increasing salt concentration and/or decreasing temperature. For example, a medium stringency condition could be provided by about 0.1 to 0.25 M NaCl at temperatures of about 37° C. to about 55° C., while a low stringency condition could be provided by about 0.15 M to about 0.9 M salt, at temperatures ranging from about 20° C. to about 55° C. Hybridization conditions can be readily manipulated depending on the desired results.

[0153] In other embodiments, hybridization may be achieved under conditions of, for example, 50 mM Tris-HCl (pH 8.3), 75 mM KCl, 3 mM MgCl₂, 1.0 mM dithiothreitol, at temperatures between approximately 20° C. to about 37° C. Other hybridization conditions utilized could include approximately 10 mM Tris-HCl (pH 8.3), 50 mM KCl, 1.5 mM MgCl₂, at temperatures ranging from approximately 40° C. to about 72° C.

[0154] In certain embodiments, it will be advantageous to employ nucleic acids of defined sequences of the present invention in combination with an appropriate means, such as a label, for determining hybridization. A wide variety of appropriate indicator means are known in the art, including fluorescent, radioactive, enzymatic or other ligands, such as avidin/biotin, which are capable of being detected. In preferred embodiments, one may desire to employ a fluorescent label or an enzyme tag such as urease, alkaline phosphatase or peroxidase, instead of radioactive or other environmentally undesirable reagents. In the case of enzyme tags, colorimetric indicator substrates are known that can be employed to provide a detection means that is visibly or spectrophotometrically detectable, to identify specific hybridization with complementary nucleic acid containing samples.

[0155] In general, it is envisioned that the probes or primers described herein will be useful as reagents in solution hybridization, as in PCR™, for detection of expression of corresponding genes, as well as in embodiments employing a solid phase. In embodiments involving a solid phase, the test DNA (or RNA) is adsorbed or otherwise affixed to a selected matrix or surface. This fixed, single-stranded nucleic acid is then subjected to hybridization with selected probes under desired conditions. The conditions selected will depend on the particular circumstances (depending, for example, on the G+C content, type of target nucleic acid, source of nucleic acid, size of hybridization probe, etc.). Optimization of hybridization conditions for the particular application of interest is well known to those of skill in the art. After washing of the hybridized molecules to remove non-specifically bound probe molecules, hybridization is detected, and/or quantified, by determining the amount of bound label. Representative solid phase hybridization methods are disclosed in U.S. Pat. Nos. 5,843,663, 5,900,481 and 5,919,626. Other methods of hybridization that may be used in the practice of the present invention are disclosed in U.S. Pat. Nos. 5,849,481, 5,849,486 and 5,851,772. The relevant portions of these and other references identified in this section of the Specification are incorporated herein by reference.

[0156] 2. Amplification of Nucleic Acids

[0157] Since many nucleic acids, especially mRNAs, are in low abundance, nucleic acid amplification greatly enhances the ability to assess expression. The general concept is that nucleic acids can be amplified using paired primers flanking the region of interest. The term “primer,” as used herein, is meant to encompass any nucleic acid that is capable of priming the synthesis of a nascent nucleic acid in a template-dependent process. Typically, primers are oligonucleotides from ten to twenty and/or thirty base pairs in length, but longer sequences can be employed. Primers may be provided in double-stranded and/or single-stranded form, although the single-stranded form is preferred.

[0158] Pairs of primers designed to selectively hybridize to nucleic acids corresponding to selected genes are contacted with the template nucleic acid under conditions that permit selective hybridization. Depending upon the desired application, high stringency hybridization conditions may be selected that will only allow hybridization to sequences that are completely complementary to the primers. In other embodiments, hybridization may occur under reduced stringency to allow for amplification of nucleic acids containing one or more mismatches with the primer sequences. Once hybridized, the template-primer complex is contacted with one or more enzymes that facilitate template-dependent nucleic acid synthesis. Multiple rounds of amplification, also referred to as “cycles,” are conducted until a sufficient amount of amplification product is produced.

[0159] The amplification product may be detected or quantified. In certain applications, the detection may be performed by visual means. Alternatively, the detection may involve indirect identification of the product via chemilluminescence, radioactive scintigraphy of incorporated radiolabel or fluorescent label or even via a system using electrical and/or thermal impulse signals.

[0160] A number of template dependent processes are available to amplify the oligonucleotide sequences present in a given template sample. One of the best known amplification methods is the polymerase chain reaction (referred to as PCR™) which is described in detail in U.S. Pat. Nos. 4,683,195, 4,683,202 and 4,800,159, and in Innis et al., 1988, each of which is incorporated herein by reference in their entirety.

[0161] A reverse transcriptase PCR™ amplification procedure may be performed to quantify the amount of mRNA amplified. Methods of reverse transcribing RNA into cDNA are well known (see Sambrook et al., 1989). Alternative methods for reverse transcription utilize thermostable DNA polymerases. These methods are described in WO 90/07641. Polymerase chain reaction methodologies are well known in the art. Representative methods of RT-PCR are described in U.S. Pat. No. 5,882,864.

[0162] Whereas standard PCR usually uses one pair of primers to amplify a specific sequence, multiplex-PCR (MPCR) uses multiple pairs of primers to amplify many sequences simultaneously (Chamberlan et al., 1990). The presence of many PCR primers in a single tube could cause many problems, such as the increased formation of misprimed PCR products and “primer dimers,” the amplification discrimination of longer DNA fragment and so on. Normally, MPCR buffers contain a Taq Polymerase additive, which decreases the competition among amplicons and the amplification discrimination of longer DNA fragment during MPCR. MPCR products can further be hybridized with gene-specific probe for verification. Theoretically, one should be able to use as many as primers as necessary. However, due to side effects (primer dimers, misprimed PCR products, etc.) caused during MPCR, there is a limit (less than 20) to the number of primers that can be used in a MPCR reaction. See also European Application No. 0 364 255 and Mueller & Wold (1989).

[0163] Another method for amplification is ligase chain reaction (“LCR”), disclosed in European Application No. 320 308, incorporated herein by reference in its entirety. U.S. Pat. No. 4,883,750 describes a method similar to LCR for binding probe pairs to a target sequence. A method based on PCR™ and oligonucleotide ligase assay (OLA), disclosed in U.S. Pat. No. 5,912,148, may also be used.

[0164] Alternative methods for amplification of target nucleic acid sequences that may be used in the practice of the present invention are disclosed in U.S. Pat. Nos. 5,843,650, 5,846,709, 5,846,783, 5,849,546, 5,849,497, 5,849,547, 5,858,652, 5,866,366, 5,916,776, 5,922,574, 5,928,905, 5,928,906, 5,932,451, 5,935,825, 5,939,291 and 5,942,391, GB Application No. 2 202 328, and in PCT Application No. PCT/US89/01025, each of which is incorporated herein by reference in its entirety.

[0165] Qbeta Replicase, described in PCT Application No. PCT/US87/00880, may also be used as an amplification method in the present invention. In this method, a replicative sequence of RNA that has a region complementary to that of a target is added to a sample in the presence of an RNA polymerase. The polymerase will copy the replicative sequence which may then be detected.

[0166] An isothermal amplification method, in which restriction endonucleases and ligases are used to achieve the amplification of target molecules that contain nucleotide 5′-[α-thio]-triphosphates in one strand of a restriction site may also be useful in the amplification of nucleic acids in the present invention (Walker et al., 1992). Strand Displacement Amplification (SDA), disclosed in U.S. Pat. No. 5,916,779, is another method of carrying out isothermal amplification of nucleic acids which involves multiple rounds of strand displacement and synthesis, i.e., nick translation.

[0167] Other nucleic acid amplification procedures include transcription-based amplification systems (TAS), including nucleic acid sequence based amplification (NASBA) and 3SR (Kwoh et al., 1989; Gingeras et al., PCT Application WO 88/10315, incorporated herein by reference in their entirety). European Application No. 329 822 disclose a nucleic acid amplification process involving cyclically synthesizing single-stranded RNA (“ssRNA”), ssDNA, and double-stranded DNA (dsDNA), which may be used in accordance with the present invention.

[0168] PCT Application WO 89/06700 (incorporated herein by reference in its entirety) disclose a nucleic acid sequence amplification scheme based on the hybridization of a promoter region/primer sequence to a target single-stranded DNA (“ssDNA”) followed by transcription of many RNA copies of the sequence. This scheme is not cyclic, i.e., new templates are not produced from the resultant RNA transcripts. Other amplification methods include “race” and “one-sided PCR” (Frohman, 1990; Ohara et al., 1989).

[0169] 3. Detection of Nucleic Acids

[0170] Following any amplification, it may be desirable to separate the amplification product from the template and/or the excess primer. In one embodiment, amplification products are separated by agarose, agarose-acrylamide or polyacrylamide gel electrophoresis using standard methods (Sambrook et al., 1989). Separated amplification products may be cut out and eluted from the gel for further manipulation. Using low melting point agarose gels, the separated band may be removed by heating the gel, followed by extraction of the nucleic acid.

[0171] Separation of nucleic acids may also be effected by chromatographic techniques known in art. There are many kinds of chromatography which may be used in the practice of the present invention, including adsorption, partition, ion-exchange, hydroxylapatite, molecular sieve, reverse-phase, column, paper, thin-layer, and gas chromatography as well as HPLC. In certain embodiments, the amplification products are visualized. A typical visualization method involves staining of a gel with ethidium bromide and visualization of bands under UV light. Alternatively, if the amplification products are integrally labeled with radio- or fluorometrically-labeled nucleotides, the separated amplification products can be exposed to x-ray film or visualized under the appropriate excitatory spectra.

[0172] In one embodiment, following separation of amplification products, a labeled nucleic acid probe is brought into contact with the amplified marker sequence. The probe preferably is conjugated to a chromophore but may be radiolabeled. In another embodiment, the probe is conjugated to a binding partner, such as an antibody or biotin, or another binding partner carrying a detectable moiety.

[0173] In particular embodiments, detection is by Southern blotting and hybridization with a labeled probe. The techniques involved in Southern blotting are well known to those of skill in the art (see Sambrook et al., 1989). One example of the foregoing is described in U.S. Pat. No. 5,279,721, incorporated by reference herein, which discloses an apparatus and method for the automated electrophoresis and transfer of nucleic acids. The apparatus permits electrophoresis and blotting without external manipulation of the gel and is ideally suited to carrying out methods according to the present invention.

[0174] Other methods of nucleic acid detection that may be used in the practice of the instant invention are disclosed in U.S. Pat. Nos. 5,840,873, 5,843,640, 5,843,651, 5,846,708, 5,846,717, 5,846,726, 5,846,729, 5,849,487, 5,853,990, 5,853,992, 5,853,993, 5,856,092, 5,861,244, 5,863,732, 5,863,753, 5,866,331, 5,905,024, 5,910,407, 5,912,124, 5,912,145, 5,919,630, 5,925,517, 5,928,862, 5,928,869, 5,929,227, 5,932,413 and 5,935,791, each of which is incorporated herein by reference.

[0175] 4. Nucleic Acid Arrays

[0176] Microarrays comprise a plurality of polymeric molecules spatially distributed over, and stably associated with, the surface of a substantially planar substrate, e.g., biochips. Microarrays of polynucleotides have been developed and find use in a variety of applications, such as screening and DNA sequencing. One area in particular in which microarrays find use is in gene expression analysis.

[0177] In gene expression analysis with microarrays, an array of “probe” oligonucleotides is contacted with a nucleic acid sample of interest, i.e., target, such as polyA mRNA or total RNA from a particular tissue type. Contact is carried out under hybridization conditions and unbound nucleic acid is then removed. The resultant pattern of hybridized nucleic acid provides information regarding the genetic profile of the sample tested. Methodologies of gene expression analysis on microarrays are capable of providing both qualitative and quantitative information.

[0178] A variety of different arrays which may be used are known in the art. The probe molecules of the arrays which are capable of sequence specific hybridization with target nucleic acid may be polynucleotides or hybridizing analogues or mimetics thereof, including: nucleic acids in which the phosphodiester linkage has been replaced with a substitute linkage, such as phophorothioate, methylimino, methylphosphonate, phosphoramidate, guanidine and the like; nucleic acids in which the ribose subunit has been substituted, e.g., hexose phosphodiester; peptide nucleic acids; and the like. The length of the probes will generally range from 10 to 1000 nts, where in some embodiments the probes will be oligonucleotides and usually range from 15 to 150 nts and more usually from 15 to 100 nts in length, and in other embodiments the probes will be longer, usually ranging in length from 150 to 1000 nts, where the polynucleotide probes may be single- or double-stranded, usually single-stranded, and may be PCR fragments amplified from cDNA.

[0179] The probe molecules on the surface of the substrates will correspond to selected genes being analyzed and be positioned on the array at a known location so that positive hybridization events may be correlated to expression of a particular gene in the physiological source from which the target nucleic acid sample is derived. The substrates with which the probe molecules are stably associated may be fabricated from a variety of materials, including plastics, ceramics, metals, gels, membranes, glasses, and the like. The arrays may be produced according to any convenient methodology, such as preforming the probes and then stably associating them with the surface of the support or growing the probes directly on the support. A number of different array configurations and methods for their production are known to those of skill in the art and disclosed in U.S. Pat. Nos. 5,445,934, 5,532,128, 5,556,752, 5,242,974, 5,384,261, 5,405,783, 5,412,087, 5,424,186, 5,429,807, 5,436,327, 5,472,672, 5,527,681, 5,529,756, 5,545,531, 5,554,501, 5,561,071, 5,571,639, 5,593,839, 5,599,695, 5,624,711, 5,658,734, 5,700,637, and 6,004,755.

[0180] Following hybridization, where non-hybridized labeled nucleic acid is capable of emitting a signal during the detection step, a washing step is employed where unhybridized labeled nucleic acid is removed from the support surface, generating a pattern of hybridized nucleic acid on the substrate surface. A variety of wash solutions and protocols for their use are known to those of skill in the art and may be used.

[0181] Where the label on the target nucleic acid is not directly detectable, one then contacts the array, now comprising bound target, with the other member(s) of the signal producing system that is being employed. For example, where the label on the target is biotin, one then contacts the array with streptavidin-fluorescer conjugate under conditions sufficient for binding between the specific binding member pairs to occur. Following contact, any unbound members of the signal producing system will then be removed, e.g., by washing. The specific wash conditions employed will necessarily depend on the specific nature of the signal producing system that is employed, and will be known to those of skill in the art familiar with the particular signal producing system employed.

[0182] The resultant hybridization pattern(s) of labeled nucleic acids may be visualized or detected in a variety of ways, with the particular manner of detection being chosen based on the particular label of the nucleic acid, where representative detection means include scintillation counting, autoradiography, fluorescence measurement, calorimetric measurement, light emission measurement and the like.

[0183] Prior to detection or visualization, where one desires to reduce the potential for a mismatch hybridization event to generate a false positive signal on the pattern, the array of hybridized target/probe complexes may be treated with an endonuclease under conditions sufficient such that the endonuclease degrades single stranded, but not double stranded DNA. A variety of different endonucleases are known and may be used, where such nucleases include: mung bean nuclease, S1 nuclease, and the like. Where such treatment is employed in an assay in which the target nucleic acids are not labeled with a directly detectable label, e.g., in an assay with biotinylated target nucleic acids, the endonuclease treatment will generally be performed prior to contact of the array with the other member(s) of the signal producing system, e.g., fluorescent-streptavidin conjugate. Endonuclease treatment, as described above, ensures that only end-labeled target/probe complexes having a substantially complete hybridization at the 3′ end of the probe are detected in the hybridization pattern.

[0184] Following hybridization and any washing step(s) and/or subsequent treatments, as described above, the resultant hybridization pattern is detected. In detecting or visualizing the hybridization pattern, the intensity or signal value of the label will be not only detected but quantified, by which is meant that the measured signal from each hybridization spot is compared to a unit value from the signal emitted by a known number of end-labeled target nucleic acids to obtain an absolute count of the copy number.

[0185] V. Pharmaceutical Formulations and Routes of Administration

[0186] It will be necessary to prepare pharmaceutical compositions in a form appropriate for use in vivo. Generally, this will entail preparing gene therapy vectors that are essentially free of pyrogens, as well as other impurities that could be harmful to humans or animals.

[0187] The phrase “pharmaceutically or pharmacologically acceptable” refers to molecular entities and compositions that do not produce adverse, allergic, or other untoward reactions when administered to an animal or a human. As used herein, “pharmaceutically acceptable carrier” includes any and all solvents, dispersion media, coatings, antibacterial and antifungal agents, isotonic and absorption delaying agents and the like. The use of such media and agents for pharmaceutically active substances is well known in the art. Supplementary active ingredients also can be incorporated into the compositions.

[0188] Administration of these compositions according to the present invention will be via any common route so long as the target tissue is available via that route. This includes intradermal, subcutaneous, intramuscular, intraperitoneal or intravenous injection. Such compositions would normally be administered as pharmaceutically acceptable compositions, described supra.

[0189] The active compounds also may be administered intranasally, intraalveolarly (inhaled), parenterally, intrathecally (into the spinal fluid compartment), intraparenchymally (into the brain or spinal cord tissues) or intraperitoneally. Solutions of the active compounds as free base or pharmacologically acceptable salts can be prepared in water suitably mixed with a surfactant, such as hydroxypropylcellulose. Dispersions can also be prepared in glycerol, liquid polyethylene glycols, and mixtures thereof and in oils. Under ordinary conditions of storage and use, these preparations contain a preservative to prevent the growth of microorganisms.

[0190] The pharmaceutical forms suitable for injectable use include sterile aqueous solutions or dispersions and sterile powders for the extemporaneous preparation of sterile injectable solutions or dispersions. In all cases the form must be sterile and must be fluid to the extent that easy administration by a syringe is possible. It must be stable under the conditions of manufacture and storage and must be preserved against the contaminating action of microorganisms, such as bacteria and fungi. The carrier can be a solvent or dispersion medium containing, for example, water, ethanol, polyol (for example, glycerol, propylene glycol, and liquid polyethylene glycol, and the like), suitable mixtures thereof, and vegetable oils. The proper fluidity can be maintained, for example, by the use of a coating, such as lecithin, by the maintenance of the required particle size in the case of dispersion and by the use of surfactants. The prevention of the action of microorganisms can be brought about by various antibacterial an antifungal agents, for example, parabens, chlorobutanol, phenol, sorbic acid, thimerosal, and the like. In many cases, it will be preferable to include isotonic agents, for example, sugars or sodium chloride. Prolonged absorption of the injectable compositions can be brought about by the use in the compositions of agents delaying absorption, for example, aluminum monostearate and gelatin.

[0191] Sterile injectable solutions are prepared by incorporating the active compounds in the required amount in the appropriate solvent with various of the other ingredients enumerated above, as required, followed by filtered sterilization. Generally, dispersions are prepared by incorporating the various sterilized active ingredients into a sterile vehicle which contains the basic dispersion medium and the required other ingredients from those enumerated above. In the case of sterile powders for the preparation of sterile injectable solutions, the preferred methods of preparation are vacuum-drying and freeze-drying techniques which yield a powder of the active ingredient plus any additional desired ingredient from a previously sterile-filtered solution thereof.

[0192] For oral administration the polypeptides of the present invention may be incorporated with excipients that may include water, binders, abrasives, flavoring agents, foaming agents, and humectants.

[0193] As used herein, “pharmaceutically acceptable carrier” includes any and all solvents, dispersion media, coatings, antibacterial and antifungal agents, isotonic and absorption delaying agents and the like. The use of such media and agents for pharmaceutical active substances is well known in the art. Except insofar as any conventional media or agent is incompatible with the active ingredient, its use in the therapeutic compositions is contemplated. Supplementary active ingredients can also be incorporated into the compositions.

[0194] The compositions of the present invention may be formulated in a neutral or salt form. Pharmaceutically-acceptable salts include the acid addition salts (formed with the free amino groups of the protein) and which are formed with inorganic acids such as, for example, hydrochloric or phosphoric acids, or such organic acids as acetic, oxalic, tartaric, mandelic, and the like. Salts formed with the free carboxyl groups can also be derived from inorganic bases such as, for example, sodium, potassium, ammonium, calcium, or ferric hydroxides, and such organic bases as isopropylamine, trimethylamine, histidine, procaine and the like.

VI. EXAMPLES

[0195] The following examples are included to demonstrate preferred embodiments of the invention. It should be appreciated by those of skill in the art that the techniques disclosed in the examples which follow represent techniques discovered by the inventor to function well in the practice of the invention, and thus can be considered to constitute preferred modes for its practice. However, those of skill in the art should, in light of the present disclosure, appreciate that many changes can be made in the specific embodiments which are disclosed and still obtain a like or similar result without departing from the spirit and scope of the invention.

Example 1 Materials and Methods

[0196] RNA Isolation and Hybridization.

[0197] All samples were obtained from local or national tissue banks and were processed under full compliance with institutional IRB requirements. Recorded tissue collection times ranged from 2-15 hours post-mortem, with the averages being 4 hours for MS and 10 hours for normals. For DNA microarray analysis, total RNA was obtained from postmortem gray or white matter of lumbar spinal cord from 9 individuals (5 with MS, and 4 controls without neurologic disease, of which 2 white matter control samples yielded sufficient RNA for the study). To assess the gene expression profile of post-mortem MS spinal cords, the inventors compared 4 MS gray matter tissues to 4 gray matter controls and 5 MS white mater tissues to 2 white matter controls (Table 1).

[0198] Analysis of the MS spinal cord samples by histopathology of both gray and white matter (average autolysis time 3.2 h), using Luxol Fast Blue, Bodian, H&E stains and GFAP, lymphocyte common antigen (LCA) and CD68 immunostaining revealed sample heterogeneity with findings that ranged from little involvement to frank inflammation, demyelination, or axonal loss. The inventors isolated RNA directly from frozen spinal cord specimens using the Qiagen RNAeasy™ kit, following the manufacturer's recommendations. Briefly, frozen tissues were dissected to separate gray and white matter, followed by mortar fragmentation in the presence of liquid nitrogen. Total RNA was isolated using the Qiagen Rneasy™ kit with the modification that the upper lipid layer was entirely removed from all samples after resuspension and spinning with buffer RLT. Although this strategy led to the discard of approximately 20-40% of the RNA sample, it preserved the overall integrity of our RNA because the lipid layer is known to compromise RNA stability and quality. All RNA samples included met quality/control standards (i.e., 260/280 OD ratios>1.8 in all RNA samples, and ratio of 3′ to 5′ signal>1.7 for GAPDH and β-actin on GeneChip for RNA samples used in microarray experiments) and were used for microarray hybridization. Though it is recognized that post-mortem changes in levels of individual mRNAs presumably occurred, these were likely similar among the specimens.

[0199] The inventors then performed microarray hybridization using RNAs isolated from gray and white matter from these spinal cords, using Affymetrix protocols. DNA microarray analysis was performed using Affymetrix HuFL GeneChip probe arrays. These microarrays contain 7,070 distinct probe sets, representing approximately 6,800 human genes. Briefly, using 7-10 μg of total RNA, double-stranded cDNA was synthesized using the Superscript Choice System (Life Technologies) with the following modifications. In the first strand synthesis, the reverse transcription reaction contained a T7-(dT)₂₄ primer plus 0.1 M DTT and 10 mM dNTP mix. For second strand synthesis, E. coli DNA ligase (10 U/μl) and T4 DNA Polymerase I (10 U/μl), 10 mM dNTP mix and RNase H (2 U/μl) were used. Phenol-chloroform extraction was followed by in vitro transcription (IVT) (Ambion T7 Megascript System) with biotin labeling. IVT was performed with (1:3) biotinylated: unlabeled CTP and UTP. The Ambion T7 enzyme mix and T7 transcription buffer were added to the ds cDNA and NTP labeling mix (ATP, CTP, UTP, GTP, Bio-11-CTP and Bio-16-UTP). The NTP labeling mix was incubated for 5 hr at 37° C., and cleaned using RNeasy columns (Qiagen). Thirteen to 20 μg of fluorescently-labeled and chemically-fragmented cRNA were used for array hybridization. Fragmented cRNA and herring sperm DNA were added to the hybridization buffer containing 1.0 M NaCl, 10 mM Tris-HCL pH 7.6, and 0.01% Triton X-100.

[0200] The hybridization mixture was heated to 99° C. for 5 min., spun, and incubated at 45° C. for 5 min, and injected into the probe array cartridge. Hybridizations were carried out at 45° C. for 16 hours with mixing at 60 rpm. Following hybridization, solutions were removed, and arrays were rinsed and incubated with 0.1× ST-T (100 mM NaCl, 10 mM Tris-HCL pH 8.0, and 0.01% Triton X-100) at 50° C. for 20 min. Hybridized arrays were stained with 5.0 μg/ml streptavidin-phycoerythrin (Molecular Probes) and 2.0 mg/ml acetylated BSA (Sigma) in 1× ST-T at 40° C. for 15 min. The streptavidin-phycoerythrin step was repeated after an intermediate amplification step in which anti-streptavidin rabbit IgG antibodies and secondary biotinylated goat anti-rabbit antibodies are added to the samples. Following washes, probe arrays were scanned twice at 6 μm resolution using the GeneChip system confocal scanner.

[0201] Microarray Data Collection and Analysis.

[0202] Scanned image files were converted to mRNA expression levels using Affymetrix GeneChip3.1 software. This software assesses presence or absence of transcripts for each probe set, taking into account metrics such as background, noise, and comparison of intensities between Perfect Match (PM) and their control Mismatch (MM) probe cells. The average intensity of each microarray was scaled to a target intensity of 1500. Files containing the average difference intensity values (i.e., expression levels) for each probe set were imported into an Access database. We assigned an arbitrary minimal expression level (i.e., average difference) value of 20 to any negative or zero values prior to performing the statistical analysis.

[0203] Selection of Discriminatory Genes. Statistics.

[0204] Several statistical measures have been introduced to identify differentially expressed genes for two conditions (e.g., cancerous and normal tissues). Parametric tests such as P-value (Golub et al., 1999) and t-test (Thomas et al., 2001) are based on differences of group means, while non-parametric tests such as Wilcoxon rank sum (Mann-Whitney) test are based on differences of rank sums in groups (Thomas et al. 2001). A couple of measures such as Wilks' lambda were also proposed for the identification of discriminatory genes in multi-classes (Dudoit et al., 2001; Hwang et al., 2002). All these parametric and non-parametric statistical tests eventually use parametric distributions such as t-distribution or F-distribution. Thus, these tests may perform poorly, resulting in producing many “false positives” or even “false negatives,” due to violation of their underlying distribution assumptions. In many cases of t-test applications, it can be seen that a histogram of t-statistic values of all genes does not match with a t-distribution theoretically defined for a given number of array samples. This discrepancy between a real distribution (histogram) and a theoretical distribution leads to “false positives” or “false negatives.”

[0205] The inventors propose a novel method that employs a non-parametric empirical estimation of a distribution, kernel density estimator, for any statistical measure used to detect differential expressions of genes in two or multiple conditions (Wand and Jones, 1995). In this study, for each gene i, a log ratio (r_(i)) between expression levels of a MS sample (g_(i) ^(MS)) and the mean of healthy samples (g_(i) ^(H)) is calculated as a statistical measure, as shown in equation 1 (Lock et al. 2002). $\begin{matrix} {r_{i} = {\log_{10}\left( \frac{g_{i}^{MS}}{g_{i}^{H}} \right)}} & (1) \end{matrix}$

[0206] Then, an empirical distribution of those ratios, which can be used for the statistical hypothesis test to select differentially expressed genes, is obtained using kernel density estimator. The density for a certain ratio (r) is defined by n ratios (r_(i)) as shown in equation 2. $\begin{matrix} {{\hat{f}\left( {r;h} \right)} = {({nh})^{- 1}{\sum\limits_{i = 1}^{n}\quad {K\left( \frac{r - r_{i}}{h} \right)}}}} & (2) \end{matrix}$

[0207] Here, K is a function satisfying ∫K(x)dx=1, which is called the kernel (normal distribution in this study), and h is a positive number, usually called the bandwidth or window width. FIG. 1 shows a kernel density estimate constructed using five ratios (five “x” marks on the x-axis) with a kernel chosen to be the normal distribution with zero mean and unit variance (N(0,1)).

[0208] In FIG. 1, the solid line is the kernel density estimated from the five ratios or kernels (dotted line) each of which is centered to each ratio. Just as a bin size, called the smoothing parameter, should be correctly chosen to explore the structure or shape of the distribution, the bandwidth should be optimally determined. A small bandwidth results in an under-smoothed estimate, while a large bandwidth an over-smoothed estimate. This sensitivity of the distribution shape to the bandwidth size is called variance-bias tradeoff. The optimal bandwidth is selected to minimize the mean integrated squared error (MISE) between the estimated density ({circumflex over (ƒ)}) and the target density (ƒ) for the kernel N(0,1), as shown in equation 3. $\begin{matrix} {\hat{h} = {\left\lbrack \frac{8\pi^{1/2}{R(K)}}{3{\mu_{2}(K)}^{2}n} \right\rbrack^{1/5}s}} & (3) \end{matrix}$

[0209] Here, R(K) and μ₂(K) are defined by ∫K(r)²dr and ∫r²K(r)dr, respectively, and s is the estimated standard deviation of ratios. Since this bandwidth to minimize MISE tends to be large, we tried ĥ/2, ĥ/4, and ĥ/8 to choose an optimal bandwidth among those derived from the MISE criterion in terms of the variance-bias tradeoff. In most of cases, ĥ/2 produced the optimal distribution structure (Wand and Jones, 1995). FIG. 2A shows a kernel density estimate for a MS sample where the optimal bandwidth is 0.052 and FIG. 2B shows a histogram with a bin size equivalent to the determined bandwidth. The kernel estimate indicates that there are two clear modes and one weak mode in the distribution. One clear mode in the left and one weak mode in the right of the distribution imply that there are more down-regulated genes in MS than up-regulated genes. Also, the mode in the center means that the majority of genes are not differentially expressed in MS and healthy patients. Comparing the kernel density estimate with the histogram, we can see that this estimated distribution matches well with the histogram.

[0210] With this empirically estimated distribution, a typical two-tailed hypothesis test is performed, as the typical t-test is done with t-distribution. The null hypothesis (H₀) is that means are equal and the alternative hypothesis (H₁) is that means are not equal. For instance, for a ratio marked on the x-axis in FIG. 2A, the area under the distribution below the ratio (a_(i) in equation 4) is calculated, and then the probability (called significance) of observing the given result by chance, when the null hypothesis is true, is determined as shown in equation 4.

p _(i)=2min(a _(i),1−a _(i))  (4)

[0211] All of the compositions and methods disclosed and claimed herein can be made and executed without undue experimentation in light of the present disclosure. While the compositions and methods of this invention have been described in terms of preferred embodiments, it will be apparent to those of skill in the art that variations may be applied to the compositions and methods and in the steps or in the sequence of steps of the method described herein without departing from the concept, spirit and scope of the invention. More specifically, it will be apparent that certain agents which are both chemically and physiologically related may be substituted for the agents described herein while the same or similar results would be achieved. All such similar substitutes and modifications apparent to those skilled in the art are deemed to be within the spirit, scope and concept of the invention as defined by the appended claims.

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What is claimed is:
 1. A method for treating or preventing multiple sclerosis (MS) comprising administering to a subject with MS a composition that causes an increase in the activity or expression of at least one gene product selected from the group consisting of those genes indicated by a minus (−) sign in Tables 1-15, other than those indicated by an asterisk.
 2. The method of claim 1, further comprising a second MS therapy.
 3. The method of claim 2, wherein the second MS therapy is given before the composition.
 4. The method of claim 2, wherein the second MS therapy is given after the composition.
 5. The method of claim 2, wherein the second MS therapy is given concurrent with the composition.
 6. The method of claim 2, wherein said second MS therapy is interferon β1a, interferon β1b, glatiramer acetate, and mitoxantrone.
 7. The method of claim 1, wherein the composition comprises peptide.
 8. The method of claim 1, wherein the composition comprises a small molecule.
 9. The method of claim 1, wherein the composition is an organo-pharmaceutical.
 10. The method of claim 1, wherein the composition comprises an expression cassette comprising a nucleic acid encoding the selected gene product and a promoter active in eukaryotic cells, said nucleic acid operably linked to said promoter.
 11. The method of claim 10, wherein said nucleic acid is comprised in a non-viral vector.
 12. The method of claim 10, wherein said nucleic acid is comprised in a viral vector.
 13. The method of claim 12, wherein said viral vector is an adenoviral vector, an adeno-associated viral vector, a retroviral vector, a herpesviral vector, a vaccinia viral vector or a polyoma viral vector.
 14. The method of claim 10, wherein said promoter is a constitutive promoter, a tissue specific promoter or an inducible promoter.
 15. The method of claim 14, wherein the tissue specific promoter is a neuronal cell promoter, a glial cell promoter, a monocyte promoter, a lymphocyte promoter, or a B cell promoter.
 16. The method of claim 10, wherein said expression cassette further comprises a polyadenylation signal.
 17. The method of claim 1, wherein said composition is administered intradermally, subcutaneously, intramuscularly, intraperitoneally, intravenously, intranasally, intraalveolarly, parenterally, intrathecally, intraparenchymally or intraperitoneally.
 18. The method of claim 1, wherein said composition is administered to said mammal more than once.
 19. The method of claim 1, wherein said composition is administered to said mammal in discrete repeated dosings.
 20. The method of claim 1, wherein the at least one gene product comprises ORF E7 from papillomavirus 5b genome homolog (D26561), interferon-inducible peptide precursor 16-Jun (U22970), cadherin FIB1 (AB000895), cyclophilin-like protein Cyp-60 (U37219), and interferon α-inducible protein p27 (X67325).
 21. The method of claim 1 or 20, wherein at least one gene product comprises cyclin E (X95406), thymocyte antigen CD1a (M28825), serine protease inhibitor p19 (U71364), and skeletal muscle troponin T (M21984).
 22. The method of claims 20, or 21, wherein the at least one gene product further comprises IFNA (interferon alpha-d) (J00210), Interferon-alpha receptor (J03171), Interferon-inducible protein 27-Sep (J04164), Interferon regulatory factor 3 (Z56281), Interferon-induced 17-kDa/15-kDa protein (M13755), Interferon-inducible and MXA homolog p78 protein (M33882), Interferon-inducible 56 Kd protein (M24594), IFN-inducible 1-8D (X57351), Tumor necrosis factor type 1 receptor associated protein TRAP1 (U12595), granulocyte-macrophage colony stimulating factor CSF1 (M13207), TGF-beta superfamily protein (AB000584), Lipoxygenase (J03600), Myeloid cell differentiation protein (MCL1) (L08246), Chemokine TARC (D43767), CD110 protein (Y10506), CD152/CTLA4 (Y10514), Thrombospondin 2 (HG896-HT896), IgG Fc binding protein (D84239), Skin-antimicrobial-peptide 1 (SAP1) (Z71389), Mac-2 binding protein (L13210), Interleukin 1 receptor (M27492), Histone H1x (D64142), Histone H3.1 (M60746), Histone H4 (M16707), H4 histone (X60486), NBPhox (D82344), HOX2G (X16667), HOX4D (X59373), HOX11 (S38742), Androgen regulated homeobox protein (NKX3 1) (U80669), Paired-box protein (PAX2) (M89470), DNA-binding protein (GLI3) (M57609), Stat2 (U18671), Transcription factor ISGF-3 (M97935), Neurogenic basic-helix-loop-helix protein (NeuroD2) (U58681), H-neuro-d4 (U43843), Lim-Domain Transcription Factor Lim-1 (HG4318-HT4588), Cyclin D3 (M92287), Cyclin E1 (M74093), Cyclin G1 (X77794), Kinase Inhibitor P27kip1 Cyclin-Dependent (HG4258-HT4528), Cdk-inhibitor p57KIP2 (KIP2) (U22398), HsMcm6 (D84557), Retinoblastoma related protein (p107) (L14812), thymidylate synthase-inducer transcription factor LSF (U03494), 218 kD Mi-2 protein (X86691), Methyl-CpG-binding protein 2 (X99687), Androgen receptor (M23263), Retinoid X receptor beta (M84820), Orphan receptor ROR gamma (U16997), Orphan nuclear receptor (DAX1) (U31929), OTF-2 lymphoid-specific transcription factor (X13810), TRANSCRIPTION FACTOR (NFATcb) (U59736), NF-AT4c (L41067), YY1 (M77698), PLZF kruppel-like zinc finger protein (Z19002), Zinc finger protein, Hsa11 (X98833), TAFII70-alpha (L25444), RNA polymerase II associated protein RAP74 (X64037), AP-4 (S73885), Lupus p70 (Ku) autoantigen protein (J04611), Zinc Finger protein Znf155 (HG4243-HT4513), HPV16 E1 protein binding protein (U96131), E1A enhancer binding protein (E1A-F) (U18018), DNA-binding protein ABP/ZF (U82613), CCAAT transcription binding factor subunit gamma (NFY-C) (Z74792), anti-oxidant nuclear respiratory factor-1 (NRF-1) (L22454), Sodium Channel 1 (HG4593-HT4998), Sodium channel 2 (hBNaC2) (U78180), HBK2 potassium channel (X17622), Vacuolar H+ ATPase proton channel subunit (M62762), Calcium Channel, Voltage-Gated, Alpha 1e Subunit, 2 (HG3242-HT3419), Calcium Channel, Voltage-Gated, Alpha 1e Subunit, 3 (HG3242-HT4231), Beta nerve growth factor (X52599), Glial Growth Factor 2 (HG4704-HT5146), Fibroblast growth factor receptor 4 (L03840), Fibroblast Growth Factor Receptor K-Sam (HG3432-HT3621), Ciliary neurotrophic factor 1 (X55889), Heparin-binding EGF-like growth factor (M60278), Corticotropin releasing factor receptor (L23333), Connective tissue growth factor (M92934), Growth hormone releasing factor (L00137), Preprothyrotropin-releasing hormone (M63582), Proneurotensin-Proneuromedin N (U91618), Serotonin receptor (5HT1E) (M91467), 5-HT6 serotonin receptor (L41147), Serotonin 1B receptor (D10995), Calcitonin (HG2290-HT2386), Estrogen receptor-related protein (hERRa1) (L38487), m4 muscarinic acetylcholine receptor (M16405), ERF-1 (X79066), PTH-like hormone A (M24351), Dopamine DIA receptor (M85247), Dopamine D4 receptor (S76942), Glutamate transporter EAAT3 (U08989), Prepro-oxytocin-neurophysin I (OXT) (M11186), Vesicular acetylcholine transporter (U09210), Chorionic gonadotropin beta subunit (K03183), Enkephalin (J00123), Delayed rectifier potassium channel (KVLQTl-Iso5) (AF003743), Melanocortin 5 receptor (MC5R) (L27080), Thyroxine-binding globulin (M14091), GABA-A receptor, beta 1 subunit (X14767), Gamma-aminobutyric acid transporter type 3 (S75989), Strychnine binding subunit of inhibitory glycine receptor (X52008), EP3 prostanoid receptor EP3-I (S68874), Endomembrane proton pump subunit (M25809), NaK-ATPase gamma subunit (U50743), Mitochondrial ATP synthase c subunit (X69908), OXA1Hs (X80695), Electron transfer flavoprotein beta subunit (X71129), COX6B (AC002115), cytochrome c oxidase subunit VIIb (Z14244), Cytochrome b pseudo (U38268), Putative copper uptake protein hCTR2 (U83461), Transferrin (S95936), Metallothionein-I-A (K01383), Metallothionein IIa (V00594), Metallothionein III (M93311), Mitochondrial creatine kinase (CKMT) (J04469), Mitochondrial isocitrate dehydrogenase (NADP+) (X69433), Mitochondrial aspartate aminotransferase (M22632), Mitochondrial aldehyde dehydrogenase x (M63967), Aldehyde dehydrogenase type III (ALDHIII) (M74542). Aldehyde dehydrogenase 6 (U07919), Aldehyde dehydrogenase (ALDH8) (U37519), Aldehyde reductase (J04794), Oxidoreductase HHCMA56 (U13395), NAD+-isocitrate dehydrogenase (U87972), Selenoprotein P (Z11793), Salivary peroxidase (U39573), Glutathione S-transferase (GSTM5) (L02321), Glutathione S-transferase theta 2 (GSTT2) (L38503), Mitochondrial NADH-ubiquinone reductase 24 Kd subunit (M22538), Succinate dehydrogenase iron-protein subunit (sdhB) (U17886), Carnitine Calcium-Binding protein Mitochondrial (HG4749-HT5197), Heme oxygenase-2 (S34389), p38beta MAP kinase (U53442), C-Ki-Ras P21 (HG2036-HT2090), Protein kinase (MLK-3) (L32976), Kinase Myt1 (U56816), Anaplastic lymphoma kinase receptor (U66559), Receptor tyrosine kinase TrkC (U05012), G protein-coupled receptor kinase (GRK6) (L16862), G-protein coupled receptor (X95876), MEK kinase 3 (U78876), MNK1 (AB000409), JNK activating kinase (JNKK1) (U17743), FK506-binding protein (FKBP) (M34539), Insulin-stimulated protein kinase 1 (ISPK-1) (U08316), Serine Kinase Psk-H1 (HG1019-HT1019), Calcium, calmodulin-dependent protein kinase II gamma (U50360), Notch 4 (U89336), Myelin associated oligodendrocytic basic protein (D28114), Axin (AF009674), Neurofilament H (X15306), Neurofilament subunit NF-L (X05608), Neurofilament triplet L protein (U57341), Axonal transporter of synaptic vesicles (X90840), Cytokeratin 4 (X07695), Cytokeratin 17 (Z19574), K6b epidermal keratin type II (L00205), Dystroglycan (DAG1) (L19711), Macrophage capping protein (M94345), LAG-1 (X53683), Keratin type 11 (58 kD) (M21389), Skeletal muscle alpha 2 actinin (M86406), 22 kDa smooth muscle protein (SM22) (M95787), Myf-4 (X17651), and MYF6 (X5201 1), Non-muscle myosin light chain MLC (M22919), 815A9.1 myosin heavy chain (AF001548), Myosin-I beta (X98507), Fibroblast muscle-type tropomyosin (M12125), Cadherin FIB1 (AB000895), Cadherin FIB2 (AB000896), Contactin (Z21488), Fibronectin (FN precursor) (X02761), Beta-2 integrin alphaD (U40279), B-cam (X80026), Alpha-1 collagen type II (M60299), elastase IIB (M16653), Basement membrane heparan sulfate proteoglycan (X62515), Guanylate kinase (GUK1) (L76200), RAD23A homolog (AD000092), Mismatch repair protein (hMLH1) (AF001359), thymidylate kinase (CDC8) (L16991), Inhibitor of apoptosis protein 1 (U45878), Lysosome-associated membrane protein-2 (S79873), GM2 activator protein (X62078), alpha mannosidase (U37248), Alpha mannosidase II isozyme (L28821), Beta-galactoside alpha-23-sialyltransferase (SIAT4A) (L13972), Gal beta-13 GalNAc alpha-23 sialyltransferase (ST3Gal II) (U63090), Gal-beta(1-3/1-4)GlcNAc alpha-23-sialyltransferase (X74570), G9 encoding sialidase (X78687), Acid sphingomyelinase (ASM) (M59916), N-acetylglucosaminyltransferase I (GlcNAc-TI) (M55621), Beta-globin (U01317), Spot14 (Y08409), Spermidine synthase (M64231), Spermidine/Spermine N1-Acetyltransferase (HG172-HT3924), Prepro-plasma carboxypeptidase B (M75106), putative purinergic receptor P2Y10 (AF000545), Ubiquitin (M26880), Semaphorin V (U28369), aminoacylase 1 (L07548), N-acetylglucosaminyltransferase V (D17716), apolipoprotein apoC-IV (U32576), Alpha topoisomerase (L47276), Azurocidin (M96326), Uridine phosphorylase (X90858), Guanine nucleotide regulatory protein (tim1) (U02082), Guanylate binding protein isom II (GBP-2) (M55543), soluble guanylate cyclase (X66534), Osteomodulin (AB000114), Deoxyuridine nucleotidohydrolase (U31930), Calcium-sensing receptor (D50855), Granule membrane protein-140 (M25322), ELAM-1 ligand fucosyltransferase (ELFT) (M58597), p52 and p64 N-Shc (D84361), Crystallin Alpha A (HG3286-HT3463), Polypeptide 7B2 (Y00757), Tax helper protein 1 (D14827), Preferentially expressed antigen of melanoma (PRAME) (U65011), MNK1 (AB000409), UDP Galactose 4 epimerase (L41668), IPL (AF001294), Carbonyl reductase (J04056), Uromodulin (Tamm-Horsfall glycoprotein) (M15881), Enigma (L35240), 40871 sequence (U72507), Endogenous retroviral protease (M27826), lrp (X79882), Phosphomevalonate kinase (L77213), Unknown function protein (AF015910), dihydrodiol dehydrogenase (U05861), Modulator recognition factor I (MRF-1) (M62324), transglutaminase (M98447), Cpg-Enriched Dna Clone S19 (HG3995-HT4265), AML1b protein (D43968), Effector cell protease receptor-1 (EPR-1) (L32866), Folylpolyglutamate synthetase (M98045), Zn-alpha2-glycoprotein (X59766), Glucose transporter-like protein-III (GLUT3) (M20681), CO-029 (M35252), Pyruvate kinase type L (M15465), Ornithine transcarbamylase (K02100), Beta-casein (X13766), DCC (deleted in colorectal cancer) (S81294), Myeloid progenitor inhibitory factor-1 MPIF-1 (U85767), Carcinoembryonic antigen (CEA) (M29540), Estrogen sulfotransferase (U55764), Paraoxonase 2 (PON2) (L48513), TESK1 (D50863), Glucokinase (GCK) (M90299), Biphenyl hydrolase-related protein (X81372), Centrin (U03270), Insulin (J00268), Calcium activated neutral protease large subunit (muCANP) (X04366), Translational initiation factor (eIF-2) alpha subunit (J02645), Oncogene M11-Af4, Fusion Activated (HG4757-HT5207), PSE-binding factor PTF gamma subunit (U44754), TIMP-3 (D45917), Zinc finger protein ZNF133 (U09366), GP-39 cartilage protein (Y08374), Transmembrane 4 superfamily protein (SAS) (U01160), Gastrin-releasing peptide (K02054), Carnitine palmitoyltransferase I type I (Y08682), HIC-1 fragment (L41919), Diacylglycerol kinase (X62535), (clone NF 10) cytochrome P-450 nifedipine oxidase (J04449), MAGE-2 (L18920), (clone F-T03796) STM-2 (L43964), Chondroitin sulfate proteoglycan (MCSP) (X96753), Importin alpha 6 (AF005361), RNAse A (D26129), Peripherin (PRPH) (L14565), Treacher Collins syndrome (TCOF1) (U76366), Aminoimidazole carboxamide ribonucleotide transmylase/inosinicase (D82348), CGM7 nonspecific cross-reacting antigen (NCA) (D90276), G9a (X69838), CLA-1 (Z22555), Mevalonate pyrophosphate decarboxylase (MPD) (U49260), Acyl-CoA thioester hydrolase (U91316), Clathrin, Light Polypeptide B (HG2797-HT2906), Tissue plasminogen activator (PLAT) (K03021), Antigen of paraneoplastic sensory neuronopathy patients (M62843), Autoantigen NOR-90 (X56687), MAC30 (L19183), Dihydroorotate dehydrogenase (M94065), Neogenin (U61262), T-Plastin (HG2755-HT2862), Sarcolipin (SLN) (U96094), Fetal apolipoprotein AI precursor (X01038), Short-chain alcohol dehydrogenase family (D82061), 8-oxo-dGTPase (D16581), 4-aminobutyrate aminotransferase (S75578), RNase 4 (D37931), Glucose-6-phosphatase (U01120), ADP-ribosyltransferase (S74683), MHC Class I region proline rich protein (U63336), Achaete scute homologous protein (ASH1) (L08424), HFREP-1 (D14446), Ectodermal dysplasia protein (EDA) (U59228), Kruppel related zinc finger protein (HTF10) (L11672), DNA polymerase delta catalytic subunit (M80397), Elongin A (L47345), Succinate dehydrogenase iron-protein subunit (sdhB) (U17886), Ret Transforming (HG2825-HT2949), Proline-Rich protein Prb4 (HG4490-HT4876), S100A2 (Y07755), Nuclear factor erythroid 2 isom f (S77763), I-plastin (L20826), Gastrin releasing peptide receptor (GRPR) (M73481), Proto-onco Wnt7a (U53476), Farnesol receptor HRR-1 (U68233), P1-Cdc21(X74794), MSX-2 (D89377), secretin receptor (U28281), LDLC (Z34975), Methylenetetrahydrofolate Reductase (HG4234-HT4504), 6-pyruvoyl-tetrahydropterin synthase (D17400), ASM-like phosphodiesterase 3b (Y08134), Placental bikunin (U78095), Xanthine Dehydrogenase (HG3288-HT3465), Intestinal mucin (MUC2) (L21998), Secreted epithelial tumour mucin antigen (X52228), Profilin II (L10678), Fatty acids omega-hydroxylase (cytochrome P-450HKV) (D13705), HU-K4 (U60644), TCTEL1 (D50663), ITBA2 protein (X92896), PEP19 (PCP4) (U52969), Argininosuccinate synthetase (X01630), Expressed pseudo TCTA at t(1;3) translocation site (L41143), 6-phosphofructo-2-kinase/fructose-26-bisphosphatase (X52638), DROER homolog (D85758), Peroxisomal L-alanine:glyoxylate aminotransferase (X53414), X11 protein (U79255), PD-ECGF/TP (S72487), PBX2 (X59842), transcobalamin II (TCN2) (L02648), Palmitoylated erythrocyte membrane protein (MPP1) (M64925), Heat shock protein E coli DnaJ homolog (L08069), Int-1 mammary oncogene (X03072), Gravin (U81607), Glyoxalase II (X90999), and MURR1 (D85433), Alpha satellite and satellite 3 junction DNA sequence (M21305), ORF (M68864), Pregnancy-specific beta-1-glycoprotein PSGGA (M37755), LIMK-2 (D45906), A33 antigen precursor (U79725), Neuroendocrine-dlg (NE-dlg) (U49089), Nucleolar protein HNP36 (X86681), Mucin 3, Intestinal (HG2147-HT2217), B-cell pseudoautosomal boundary-like sequence (D55638), ELAM-1 ligand fucosyltransferase (ELFT) (M58597), Factor VII serine protease precursor (M13232), EPC-1 (U57450), 17 beta hydroxysteroid dehydrogenase type 2 (L 11708), Ini1 (U04847), Nup88 (Y08613), Cysteine protease CPP32 isom alpha (U13737), Int-2 protooncogene (X14445), GRB-7 SH2 domain (D43772), SH3 binding RES4-23A (AB000462), Platelet glycoprotein IIb (GPIIb) (M34344), R2 inducible membrane protein (X53795), MUC6 (HG880-HT880), RING protein (Y07829), EYA3 (Y10262), Prostasin (L41351), Lambda/iota-prot kinase C-interacting protein (U32581), EYA1 (Y10260), BENE (U17077), Prolargin (PRELP) (U41344), HRX-like protein (Y08836), Alpha-1-Antitrypsin (HG3517-HT3711), and ATP-binding cassette protein (U18237).
 23. The method of claims 20, or 21, wherein the at least one gene product further comprises KIAA0176 (D79998), KIAA0123 (D50913), KIAA0320 (AB002318), KLAA0198 (D83784), KIAA0163 (D79985) and KLAA0246 (D87433), KIAA0028 (D21851), KIAA0224 (D86977), KIAA0018 (D13643), KIAA0113 (D30755), KIAA0011 (D13636), KIAA0181 (D80003), KIAA0182 (D80004), and KIAA0317 (AB002315), KIAA0159 (D63880), KIAA0384 (AB002382), KIAA0207 (D86962), KIAA0175 (D79997), KIAA0049 (D30756), KIAA0061 (D31765), KIAA0154 (D63876), KIAA0109 (D63475), KIAA0057 (D31762), KIAA0186 (D80008), KIAA0006 (D13631), KIAA0095 (D42085), KIAA0192 (D83783), KIAA0199 (D83782), KIAA0263 (D87452), KIAA0140 (D50930), KIAA0048 (D28588), KIAA0040 (D25539), KIAA0008 (D13633), KIAA0030 (D21063), KIAA0051 (D29640), KIAA0153 (D63487), KIAA0144 (D63478), KIAA9001 (D42040), KIAA0107 (D14663), KIAA0118 (D42087), KIAA0130 (D50920), and KIAA0167 (D79989).
 24. The method of claim 1, further comprising modulating the level of a gene product in Tables 16, 17 or 18, or CD18.
 25. A method for treating or preventing multiple sclerosis (MS) comprising administering to a subject with MS a composition that causes a decrease in the activity level or expression of a gene product selected from the group consisting of those genes indicated by a plus (+) sign in Tables 1-15, other than those indicated by an asterisk.
 26. The method of claim 25, further comprising a second MS therapy.
 27. The method of claim 26, wherein the second MS therapy is given before the composition.
 28. The method of claim 26, wherein the second MS therapy is given after the composition.
 29. The method of claim 26, wherein the second MS therapy is given concurrent with the composition.
 30. The method of claim 26, wherein said second MS therapy is interferon β1a, interferon β1b, glatiramer acetate, and mitoxantrone.
 31. The method of claim 25, wherein the composition comprises peptide.
 32. The method of claim 25, wherein the composition comprises a small molecule.
 33. The method of claim 25, wherein the composition is an organo-pharmaceutical.
 34. The method of claim 25, wherein the composition comprises an expression cassette comprising a nucleic acid encoding an antisense construct or a ribozyme targeting the selected gene product, and a promoter active in eukaryotic cells, said nucleic acid operably linked to said promoter.
 35. The method of claim 34, wherein said nucleic acid is comprised in a non-viral vector.
 36. The method of claim 34, wherein said nucleic acid is comprised in a viral vector.
 37. The method of claim 36, wherein said viral vector is an adenoviral vector, an adeno-associated viral vector, a retroviral vector, a herpesviral vector, a vaccinia viral vector or a polyoma viral vector.
 38. The method of claim 34, wherein said promoter is a constitutive promoter, a tissue specific promoter or an inducible promoter.
 39. The method of claim 38 wherein the tissue specific promoter is a neuronal cell promoter, a glial cell promoter, a monocyte promoter, a lymphocyte promoter, or a B cell promoter.
 40. The method of claim 34, wherein said expression cassette further comprises a polyadenylation signal.
 41. The method of claim 25, wherein said composition is administered intradermally, subcutaneously, intramuscularly, intraperitoneally, intravenously, intranasally, intraalveolarly, parenterally, intrathecally, intraparenchymally or intraperitoneally.
 42. The method of claim 25, wherein said composition is administered to said mammal more than once.
 43. The method of claim 25, wherein said composition is administered to said mammal in repeated discrete dosings.
 44. The method of claim 25, where the at least one gene product comprises autoantigen calreticulin (M84739), ubiquitin-conjugating enzyme (UBE2I) (U45328), Wiskott-Aldrich syndrome protein (WASP) (U12707), placental type alkaline phosphatase (ALP-1) (J04948), and extracellular-superoxide dismutase (SOD3) (J02947).
 45. The method of claim 25 or 44, where the at least one gene product comprises Protein tyrosine phosphatase sigma (U35234), expressed pseudo T-cell leukemia translocation-associated (TCTA) (L41143), Alpha1(XI) collagen (COL11A1) (U12139), Tyk2 non-receptor protein tyrosine kinase (X54637), and Spliceosomal protein Sap 62 (HG3033-HT3194).
 46. The method of claim 25 or 44, where the at least one gene product comprises anti-B cell autoantibody IgM heavy chain variable VDJ region (U24683), Ig Heavy Chain, Vdjrc Regions (HG3731-HT4001), Ig-related 14.1 protein (M27749), Omega light chain protein 14.1 (Ig lambda chain related) (M34516), IGHA1 from Ig germline H-chain G-E-A region A: gamma-3 5 (J00220), Fc-gamma-RIIA IgG Fc receptor class IIA (X68090), Fc Receptor Iib3 For Igg, Low Affinity (HG491-HT491), Ig-like transcript 2 (U82279), Ig Heavy Chain Vdjc Regions (HG4458-HT4727), Ig J chain (M12759), and Ig alpha 2=Ig A heavy chain allotype 2; Also: S55735 (S71043).
 47. The method of claim 44, 45, or 46, wherein the at least one gene product further comprises NRAMP1 (D50402), Leukocyte adhesion protein (LFA-1/Mac-1) (M15395), T cell receptor zeta-chain (J04132), T-cell receptor T3 gamma polypeptide (X04145), Interferon (IFN-alpha-M1) (M27318), Interferon alpha IFN-alpha 6 (X02958), Alpha interferon (V00551), Interferon-gamma receptor alpha chain (U19247), Interferon gamma receptor accessory factor-1 (AF-1) (U05875), TNF receptor (M58286), Tumor Necrosis Factor Receptor 2 Associated protein Trap3 (HG4683-HT5108), IFNB 1 (V00535), IL-4 splice variant (X81851), Interleukin-6-receptor (X58298), Interleukin-8 receptor type B (IL8RB)/U11877 (U11877), Interleukin-15 receptor alpha chain precursor (IL15RA) (U31628), Complement component 2 (C2) allele b (L09708), Complement component C9 (X02176), Adipsin/complement factor D (M84526), Complement component properdin; Also: X57748 (M83652), C5a anaphylatoxin receptor (M62505), Lipocortin (X05908), Beta-hexosaminidase beta-subunit (HEXB) (M23294), L-histidine decarboxylase (D16583), GPSAT=glycophorin SAT; Also: L31860 (S77893), Tyrosine Kinase Receptor Axl 2 (HG162-HT3165), Phospholipid Transfer protein (HG3945-HT4215), MHC class I-related protein; Also: X91625, U65416, X92841 (L14848), MHC class II HLA-DP light chain (M57466), MHC class II HLA-DR-beta-1*09012 (HLA-DRB1*09012) (M96132), MBP-2 MHC binding protein 2 (X65644), Platelet/endothelial cell adhesion molecule-1 (PECAM-1) (L34657), ME491/CD63 antigen (X62654), Heat shock protein hsp40 homolog (U40992), Heat-shock protein HSP70B′ (X51757), Thromboxane synthase (M80647), Thromboxane A2 receptor (D38081), Thrombospondin 2 (HG896-HT896), Granulocyte colony-stimulating factor receptor (CSF3R) (M59820), Plasminogen activator inhibitor type 1 N-terminus (X04729), Autoimmune Antigen Thyroid Disease-Related Antigen (HG3578-HT3781), Integrin beta-5 subunit (X53002), Integrin beta 7 subunit (S80335), Neuronal PAS1 (NPAS1) (U77968), Prointerleukin 1 beta (X04500), Interleukin 1 receptor antagonist IRAP (X53296), R kappa B (U08191), Cathepsin C (X87212), Lymphocyte Antigen Hla-G3 (HG273-HT273), Lymph node homing receptor (M25280), Monocyte chemoattractant protein-4 precursor (MCP-4) (U46767), thymosin beta (D82345), Tissue inhibitor of metalloproteinase 4 (U76456), Pancreatic phospholipase A-2 (PLA-2) (M21056), Fetal brain adenylyl cyclase (L05500), Adenylyl cyclase (L21993), Guanine nucleotide-binding protein (Gi) alpha subunit (M27543), Type 2 inositol 1 4 5-trisphosphate receptor (D26350), Putative G protein-coupled receptor (AZ3B); Also:U62027 (U28488), GNAT1 transducin alpha-chain (X15088), Transducin beta-2 subunit (M36429), Transducin-like enhancer protein (TLE3) (M99438), Low-Mr GTP-binding protein (RAB31) (U59877), 43 kDa inositol polyphosphate 5-phosphatase (Z31695), RAB7 (X93499), Ras Inhibitor Inf (HG511-HT511), R-ras (M14949), RasGTPase activating protein (D78156), Clone 110298 (L43579), Rab GDI (D13988), RhoE=26 kda GTPase homolog (S82240), HSPDE4C1 3 ,5-cyclic AMP phosphodiesterase (Z46632), SLP-76 associated protein (U93049), Calmodulin (M19311), Calmodulin dependent phosphodiesterase PDE1B1 (U56976), Calcineurin A catalytic subunit (S46622), Cyclophilin C (S71018), Cyclophilin-like protein (U37221), Secreted cyclophilin-like protein (SCYLP) (M63573), Fk506-Binding protein (HG1139-HT4910), Phospholipase C (M37238), GTPase activating protein (rap1GAP) (M64788), RasGTPase activating protein (D78156), Ras-Specific Guanine Nucleotide-Releasing Factor (HG2510-HT2606), Ras-related protein Rab5b (X54871), Ras inhibitor (Rin1) (L36463), RIN protein (Y07565), Guanine Nucleotide-Binding protein Rap2 (HG1996-HT2044), Guanine nucleotide-binding protein (Gi) alpha subunit (M27543), Guanine nucleotide-binding protein G-s-alpha-3 (M21142), Small G protein (Gx) (M64595), pp52=B lymphocyte signal transduction (S58733), GPR3 G protein-coupled receptor (U18550), Dishevelled homolog (DVL) (U46461), Protein kinase C delta-type (D10495), ERK6 extracellular signal regulated kinase (X79483), Tyrosine kinase (TXK) (L27071), Serine/Threonine Kinase (HG2709-HT2805), Tyrosine kinase (ELK1) (M25269), Casein kinase I gamma 2 (U89896), Calcium, calmodulin-dependent protein kinase II gamma (U50360), ERK6 extracellular signal regulated kinase (X79483), Serine/threonine kinase MNB (mnb) (U52373), T cell-specific tyrosine kinase (L10717), (clone FBK III 11c) protein-tyrosine kinase (DRT) (L41939), Phosphorylase kinase (PSK-C3) (M31606), p35 regulatory subunit of cdk5 kinase (X80343), 40 kDa protein kinase related to rat ERK2 (Z11695), PCTAIRE-3 serine/threonine protein kinase (X66362), Protein-tyrosine-phosphatase D1 (X79510), Tyrosine Phosphatase 1; Also: U12128 (HG3187-HT3366), Protein tyrosine phosphatase delta (L38929), Protein phosphatase 2A alpha subunit (M64929), Fructose 6-phosphate 2-kinase/fructose 2 6-bisphosphatase (D49817 and D49818), Inositol polyphosphate 1-phosphatase (L08488), Protein phosphatase 5 (X89416), Protein phosphatase X (X70218), InsP3 5-phosphatase; Also: Z31695 (X77567), Putative G protein-coupled receptor (AZ3B) (U28488), Cyclic nucleotide phosphodiesterase PDE2A3 (U67733), RGS3 (AF006609), Beta catenin/TCF-4 (Y11306), Nicotinic acetylcholine receptor alpha4 subunit precursor (U62433), Alpha-A1-adrenergic receptor (M76446), Beta 4 nicotinic acetylcholine receptor subunit (U48861), m3 muscarinic acetylcholine receptor (CHRM3) (U29589), Olfactory receptor cluster (U58675), Vasopressin V1b receptor (D31833), 43 kD acetylcholine receptor-associated protein (Rapsyn) (Z33905), Atrial natriuretic factor (M54951), Monoamine oxidase A (MAOA) (M68840), Transcobalamin I (J05068), Cholecystokinin type A receptor (CCK-A) (U23430), Growth hormone-releasing hormone receptor (L01406), Follicle stimulating hormone receptor (M65085), Chorionic gonadotropin beta subunit (K03189), CB2 (peripheral) cannabinoid receptor (X74328), Beta-2-adrenergic receptor (M15169), Spasmolytic polypeptide (SP) (X51698), Thyroid transcript factor 1 (X82850), Platelet factor 4 (PF4) (M25897), Preproinsulin; Also: M10039 (V00565), Insulin-like growth factor binding protein 5 (IGFBP-5) (M65062), IGF binding protein complex acid-labile subunit a (M86826), Glucagon-like peptide-1 receptor with CA dinucleotide repeat (U01157), Choline Acetyltransferase (HG4051-HT4321), hIRS-1=rat insulin receptor substrate-1 homolog (S85963), NMDA receptor modulatory subunit 2A (hNR2A) (U09002), Metabotropic glutamate receptor 4; Also: X80818 (U92457), Excitatory amino acid transporter 4 (U18244), PephBGT-1 betaine-GABA transporter (U27699), Corticotropin releasing factor receptor (L23333), Parathyroid hormone-related protein (M17183), Somatostatin receptor subtype 3 (SSTR3); Also: Z86000 (M96738), T3 receptor-associating cofactor-1; Also: U37146 (S83390), Telencephalin precursor (U72671), (clone CR-3) teratocarcinoma-derived growth factor 3 TDGF3 (M96956), P2× purinoceptor (AF000234), P2X7 receptor (Y09561), Group-specific component vitamin D-binding protein (M11321), Thymidylate kinase (CDC8) (L16991), DNA-repair protein (XRCC1) (M36089), Replication factor C 37-kDa subunit (M87339), Sox3 (X71135), SOX-4 protein (X70683), SOX5=Sry-related HMG box (S83308), RAD51 (D14134), Mutator (hMSH2) (U03911), Cdc25A (M81933), RBP2=retinoblastoma binding protein 2 (S66431), SWI/SNF complex 60 KDa subunit (BAF60c) (U66619), Retinoic acid receptor gamma 1 (M38258), Cellular retinoic acid-binding protein (S74445), Cyclin I (D50310), Checkpoint suppressor 1 (U68723), Cell cycle checkpoint control protein (U53174), PRAD1 cyclin (X59798), Cyclin F (Z36714), CCG1/TFIIDp250 (D90359), (clone mf18) RNA polymerase II (L37127), TFIIIC Box B-binding subunit (U02619), Ets domain protein ERF (U15655), Myelin TRANSCRIPTION FACTORS 1 (MTF1) (M96980), Paired Box Hup1 (HG2188-HT2258), Homeotic protein Hox54 (HG3502-HT3696), Homeobox (clone HHO.c13); Also: X17360 (X04706), HOX 5.1 protein (X17360), Homeobox protein (PHOX1) (M95929), Homeotic protein Hpx-42 (HG3884-HT4154), Khead Family Afx1 (HG4245-HT4515), AFX protein (X93996), PAX3B=transcription factor; Also: S69369 (S69370), Pur (pur-alpha) (M96684), HOX7 (M76732), Delta opioid receptor (U07882), Nuclear orphan receptor LXR-alpha (U22662), PAX3A=TRANSCRIPTION FACTOR (S69369), Basic Transcription Factor 44 Kda Subunit (HG3748-HT4018), B-cell specific TRANSCRIPTION FACTOR (BSAP) (M96944), Nucleolar autoantigen No 55 (U47621), Transcription elongation factor (SII) (M81601), Polyadenylate binding protein II (Z48501), ERF-2 (X78992), DNF1552 (lung) (J03068), High mobility group protein HMG-I(Y) (L17131), Putative HMG-17 non-histone protein (X13546), B-myb (X13293), Erythroid-specific TRANSCRIPTION FACTORS EKLF (U65404), Faciogenital dysplasia (FGD1) (U11690), Br140(M91585), MSS1 (D11094), Nuclear factor I-X (L31881), Zn-15 related zinc finger protein (rlf) (U22377), Id-related helix-loop-helix protein Id4 (U28368), DNA-binding protein (HRC1) (M91083), DNA binding protein (HPF2) (M27878), Indian hedgehog protein (IHH) (L38517), PBX2 (X59842), Transcription Factor Btf3 Homolog M90355 (HG4518-HT4921), Proto-Oncogene C-Myc (HG3523-HT4899), Spi-1 proto-oncogene (X52056), Spi-B (X66079), Proliferating cell nuclear antigen (PCNA) promoter region (J05614), p50-NF-kappa B homolog (S76638), Basic TRANSCRIPTION FACTOR 62 kD subunit (BTF2) (M95809), Basic Transcription Factor 44 Kda Subunit (HG3748-HT4018), TRANSCRIPTION FACTOR SIM2 short form (U80457), C-kit proto-oncogene (X06182), Id-related helix-loop-helix protein Id4 (U28368), C/EBP gamma (U20240), Interleukin-1 beta convertase (IL1BCE, CASPASE 1) (M87507), DNA (cytosin-5)-methyltransferase (X63692), RNA polymerase subunit hRPB 33 (J05448), Inducible poly(A)-binding protein (U33818), H12 histone H1 (X57129), H2B/h/Z80780 (Z80780), H4/h H4 histone (X60487), Myeloid elf-1 like factor (MEF) (U32645), TRANSCRIPTION FACTOR GATA-2 (M77810), NBK apoptotic inducer protein (X89986), L-type calcium channel (Z26256), CNG2=cyclic nucleotide-gated cation channel/S76067 (S76067), Vacuolar H+-ATPase (L35249), K+ channel beta 2 subunit (U33429), Epithelial amiloride-sensitive sodium channel gamma (X87160), Channel-like integral membrane protein (CHIP28) (M77829), K-C1 cotransporter (hKCC1) (U55054), Voltage-gated calcium channel beta subunit (U07139), DHP-sensitive calcium channel gamma subunit (CACNLG) (L07738), P/Q-type calcium channel alpha1 subunit; Also: U79663 (X99897), Acid sphingomyelinase (ASM) (M59916), N-acetylglucosaminyltransferase I (GlcNAc-TI) (M55621), Alpha (1,3) fucosyltransferase (FUT6), GalNAc-T4/Y08564 (Y08564), Acid ceramidase (U70063), Beta-galactoside alpha26-sialyltransferase (SIAT1)/U67849 (U67849), UCP1 uncoupling protein (X51954), UCP3S (U82818), Glutathione transferase M3 (GSTM3) (J05459), Selenium-binding protein (hSBP)/U29091 (U29091), Manganese superoxide dismutase SOD2 (X07834), ATL-derived factor/thioredoxin (X77584), Ceruloplasmin (ferroxidase) (M13699), FDXR (adrenodoxin reductase); Also: HG2836-HT2962 (M58509), Mitochondrial NAD(P)+ dependent malic enzyme (M55905), HALPHA44 alpha-tubulin (X06956), Alpha1(XI) collagen (COL11A1) (U12139), Alpha-1 collagen type II s 1 2 and 3 (M60299), Skeletal muscle LIM-prot SLIM2 (U60116), Beta-myosin heavy chain (M21665), Dermal fibroblast elastin (X52896), Cadherin (D88799), Cardiac troponin I (X90780), Cardiac troponin T (X74819), Chitotriosidase precursor (U29615), Apolipoprotein AII (X04898), Hair keratin hHb5 (X99140), Hair keratin hHb6 (X99142), High-sulphur keratin (X63755), Collagen Type Viii Alpha 1 (HG2614-HT2710), a1(XIX) collagen chain; Also: U09279 (D38163), Myotubularin related protein 1 (MTMR1) (U58032), Myosin VIIA (USH1B) (U39226), Beta-myosin heavy chain; Also: X52889 (M21665), Myosin, Heavy Polypeptide 10, Non-Muscle (HG2175-HT2245), Myosin; Also: M36769 (Z38133), Smooth muscle myosin heavy chain isoform Smemb (S67247), Embryonic/atrial myosin light chain (MLC-1-emb/A isoform) (M37075), High-sulphur keratin (X63755), Microtubule-associated protein 2 (MAP2) (U01828), Microtubule-associated tau protein (X14474), Alpha 1 syntrophin (S81737), Dystrobrevin-epsilon; Also: U46744 (U46746), Dynactin (U73799), Dynein HeavyChain (HG2417-HT2513), Enteric smooth muscle gamma-actin (D00654), Non-muscle alpha-actinin (M95178), Microtubule-associated protein 2 (MAP2) (U01828), Duchenne Muscular Dystrophy protein (Dmd); Also: M18533 (HG2260-HT2349), Synaptophysin (p38) (X06389), Ladinin (LAD) (U42408), Beta B1-crystallin (U35340), Cylicin (Z22780), Cylicin II (Z46788), Loricrin (M94077), Intestine-specific annexin (Z11502), Annexin V (ANX5) (U01691), Phospholipid scramblase (AF008445), BAK BCl-2 homolog (X84213), Bcl-2 binding component 3 (bbc3) (U82987), Survival motor neuron protein (U80017), Phosphoribosylpyrophosphate synthetase (X15331), Uroporphyrinogen III synthase (J03824), Muscle glycogen synthase (J04501), ATP synthase B chain (D28383), Deoxyhypusine synthase (U26266), Pyrroline 5-carboxylate synthetase (X94453), S-adenosylmethionine synthetase (D49357), G7a valyl-tRNA synthetase (X59303), Aromatase (estrogen synthetase) (X13589), PP15 (placental protein 15) (X07315), Placental protein 5 (D29992), Delta3, delta2-CoA-isomerase (L24774), Topoisomerase type II (M27504), Thyroid Peroxidase (HG2999-HT4756 or M25715), Triglyceride lipase (M29194), Hormone-sensitive lipase testicular isoform (U40002), LDL-phospholipase A2 (U24577), Carbonic anhydrase VII (CA VII) (M76424), Procarboxypeptidase A1 (X67318), Prepro-plasma carboxypeptidase B (M75106), Carboxypeptidase M (J04970), Melanocortin 5 receptor (MC5R) (L27080), PSG10 pregnancy specific glycoprotein 10 (X17098), Glutamate pyruvate transaminase (GPT) (U70732), Neurotensin receptor (X70070), hnRNP-E2 (X78136), Small Nuclear Ribonucleoprotein U1, 1snrp (HG4557-HT4962), Heterologous ribonucleoprotein A0 (U23803), Ribosomal protein L3 (X73460), XIST a (X56199), Sel-1 like (U11037), p126 (ST5) (U15131), Cleavage signal 1 protein (M61199), Membrane glycoprotein M6 (D49958), Post-synaptic density protein 95 (PSD95) (U83192), LDL-receptor related protein (X13916), Clone lambda 5 semaphorin (U33920), major transcript I (U27333), A9A2BRB7 (CAC)n/(GTG)n repeat-containing clone (U00952), Activin beta-A subunit (2) (X57579), Adducin Alpha Subunit 2 (HG651-HT4201), Gps2 (GPS2) (U28963), Involucrin (M13903), Docking protein (signal recognition particle receptor) (X06272), Tight junction (zonula occludens) protein ZO-1 (L14837), Apomucin (Z48314), Pancreatic mucin (J05582), Mucin/M22406 (HG1067-HT1067), Z68155 and others (X79683), Histo-blood group ABO protein (U15197), Hs-cul-4A (U58090), Plectin (PLEC1) (U53204), TPRC (X99720), Prolyl 4-hydroxylase alpha subunit (M24486), Prolyl 4-hydoxylase beta subunit (X05130), 4F2 glycosylated heavy chain (4F2HC) antigen (M21904), Cosmid clone LUCA17/3p213 (AC002077) clone 1D2 (Z78289), Uridine nucleotide receptor (UNR) (U40223), Pre-splicing factor SRp20(D28423), Lfp35 from BRCA1, Rho7 and vatI (L78833), p97 homolog (D85939), HIV-1 Nef interacting protein (Nip7-1) (U83843), HFH4 (X99350), XG (clone RACE5) (Z48519), LLGL (D50550), MUF1 protein (X86018), Unknown protein (clone ICRFp507O0882) (Z70220), Heregulin-beta2 (M94167), NB-1 (M58026), Caveolin (Z18951), ATP-binding cassette protein (ABC2) (U18235), SNC19 sequence (U20428), UDP-galactose transporter 2 (D88146), CE29 4.1 (CAC)n/(GTG)n repeat-containing clone (U00928), gp25L2 protein (X90872), E6-AP ubiquitin protein ligase 3A (AF002224), Ribosomal DNA repeating unit (U13369), Vacuolar proton ATPase subunit D (X71490), Inter-alpha-trypsin inhibitor subunit 3 (X16260), Leukemia virus receptor 1 (GLVR1) (L20859), Clone S171 (L40393), Clone cD24-1 Huntington's candidate region fragment (L37199), FLII (U80184), Inhibin A-subunit (M13981), K12 protein precursor (U77643), Factor X (blood coagulation factor) (L29433), M25296 and others (M31776), Chondroadherin (U96769), Clone 23933 sequence (U79273), Protein immuno-reactive with anti-PTH polyclonal antibodies (U28831), Metastasis-associated mta1 (U35113), Bleomycin hydrolase (X92106), Gu binding protein (U78524), 65 kDa hydrophobic protein (U17566), Ribosomal protein L18a Homolog (HG4390-HT4660), Terminal transferase (M 11722), Skeletal muscle LIM-protein SLIM2 (U60116), EVX1 (X60655), HNSPC (D82346), (23k/3) ubiquitin-conjugating enzyme UbcH2 (Z29331), Mg81 (HG909-HT909), Growth-arrest-specific protein (gas) (L13720), Peripheral myelin protein-22 (PMP22) 1B (U08096), Mouse transaldolase (U67611), hHKb1 protein (X81420), L-arginine:glycine amidinotransferase (X86401), Furin (X17094), UGT2BIO udp glucuronosyltransferase (X63359), Transmembrane protein Tmp21-IIex (X97444), U1 small nuclear RNP-specific C protein (X12517), Nicotinamide nucleotide transhydrogenase (U40490), Nicotinamide N-methyltransferase 1 and 5 ing region (U51010), Chymotrypsinogen (M24400), Netrin-2 like protein (NTN21) (U86759), M95971 (J05252), Phosphoprotein Tal2 (HG4068-HT4338), PAC clone DJ525N14/Xq23 (AC002086), 62 kDa paraneoplastic antigen (L02867), Transglutaminase E3 (TGASE3) (L10386), NB Neurofibromin (D12625), HIV-1 Nef interacting prot (Nip7-1) (U83843), Uterus ficolin-1 (D83920), NF-AT3 (L41066), WD protein IR10 (U57057), Beta-microseminoprotein (MSP) (M34376), Clk2 (L29218), TNNT2 11/X98482 (X98482), RR2 small subunit ribonucleotide reductase (X59618), DD96 (U21049), AP-3 complex beta3A subunit (U91931), Hemopexin (M36803), Recoverin (S62028), Cartilage matrix protein (CMP) (M55682), B56-delta (L76702), (˜95%) SFTPA2D (HG3928-HT4198), Antileukoprotease (ALP) from cervix uterus (X04470), CD171 protein (Y10207), Thyroid receptor interactor (TRIP9) (L40407), H19 RNA (spliced in silico) (M32053), (clone S171) (L40393), Unknown protein (U82306), Coronin (X89109), KIAA0055 (D29956), Telomerase reverse transcriptase (AF015950), Tigger 1 transposable element (U49973), Transcript ch132/S77361 (S77361), Low density lipoprotein receptor (M28219), Chondroitin/dermatan sulfate proteoglycan (PG40) core protein (M14219), Endometrial bleeding associated factor (U81523), Fra-2 (X16706), Phosphoglucomutase 1 (HG3893-HT4163), Steroid 11-beta-hydroxylase (CYP11B1) (M32879), RSRFR2 (X63380), Small proline rich protein (sprII), clone 174N (M21302), CHD5 protein (Y12478), Na+,K+-ATPase catalytic subunit alpha-III isoform (M37457), DP-2 (L40386), Propionyl-CoA carboxylase beta-subunit (M31169), NECDIN related protein (U35139), DNL1L from chromosome X region (L44140), GOS2 (M72885), Clones 23920 and 23921 sequence (U79271), Germline oligomeric matrix protein (COMP) (L32137), LISCH7 (liver-specific bHLH-Zip transcription factor) (AD000684), Cpg-Enriched Dna, Clone E18 (HG3991-HT4261), MADER (X70991), Bone morphogenetic protein-3b (D49493), Macrophage lectin 2 (D50532), Hereditary multiple exostosis (U96629), Erythrocyte membrane protein band 42 (EPB42) (M60298), Zinc finger protein (clone 647) (X16282), Branched chain decarboxylase alpha subunit (Z14093), Sterol regulatory element binding protein-2 (U02031), UDP-galactose translocator (D84454), Hermansky-Pudlak syndrome protein (HPS) (U65676), Ribonuclease k6 precursor/U64998 (U64998), Chromosome 12p15 BAC clone CIT987SK-99D8 sequence (U91327), Chromosome 17q12-21 clone pOV-2 (U18919), (clone p5-23-3) (L48692), Hypothetical protein Npiiy20/M76676 (HG167-HT167), Plakophilin; Also: X79293 (Z34974), 75-kD autoantigen (PM-Sc1) (M58460), High-mobility group phosphoprotein isoform I-C (HMGIC) (U28749), Alpha-1-antitrypsin-related protein (M19684), DLX-2 (Dlx2) (U51003), Blood platelet membrane glycoprotein Ib-alpha (GPIB) (M22403), Tumor-associated membrane protein homolog (TMP) (U43916), Clone A9A2BRB5 (CAC)n/(GTG)n repeat-containing (U00946), Zinc finger protein 45 (ZNF45) (L75847), Beige-like protein (BGL) (M83822), Splicing Factor Sc35 m 3 (HG3088-HT3263), HZF2 zinc finger protein (X78925), Cytosolic serine hydroxymethyltransferase (SHMT) (L11931), S-lac lectin L-14-II (LGALS2) (M87860), Angiotensin II type 2 receptor (U20860), MN1 protein (clone ICRFp507I0498); Also: X82209 (Z70218), Splicing factor, SF1-Bo isoform; Also: L49380 (Y08766), Pregnancy zone protein (X54380), Nuclear respiratory factor 1 (NRF1) (U44848), Clones MDP4 MDP7 microsomal dipeptidase (MDP) (J05257), Gastrin-binding protein/X98225 (X98225), Acrosin (EC 342110) (Y00970), Peptide Yy; Also: D13897_rna2 (HG2348-HT2444), G protein-coupled receptor (STRL22) (U68031), CGM1 (HG1728-HT1734), Cystatin D (HG1098-HT1098), (clone 353) DRAL (L42176), (clone CTG-B37) sequence (L10377), Down syndrome critical region 1 (DSCR1) alternative 1 (U85265), Zinc Finger protein Zfp-36 (HG3491-HT3685), EAR-1r (D16815), (clone s22i71) (L40396), NCBP interacting protein 1 (D59253), Erythroblastosis virus onco homolog 2 (ets-2) (J04102), BLR1 Burkitt's lymphoma receptor 1 (X68149), Trabecular meshwork-induced glucocorticoid response protein (AF001620), bHLH-PAS protein Jap3 (U60415), Guanylin (M97496), Dioxin-responsive (S81578), RD/X99296 (X99296), Plasma inter-alpha-trypsin inhibitor heavy chain H(3) (X14690), Major Yo paraneoplastic antigen (CDR2) (M63256), PCI (plasminogen activator inhibitor 3) from protein C inhibitor (M68516), KNP-Ib; Also: U53003 (D86062), MJD1=MJD1 protein {CAG repeats} (S75313), POM121-like 1 (D87002), Cell surface glycoprotein P3.58 (M55024), Oviductal glycoprotein (U09550), Kallmann syndrome (KAL) (M97252), PACAP receptor (D17516), Retinal pigment epithelium-specific 61 kDa protein (RPE65) (U18991), Squamous cell carcinoma antigen=serine protease inhibitor (S66896), Clone 23948 sequence (U79293), Albumin, 3; Also: HG2841-HT2970, HG2841-HT2968 (HG2841-HT2969), Protein containing SH3 domain SH3GL2 (X99657), HK2 hexokinase II (Z46376), Ribosomal protein S6 kinase 2 (RPS6KA2) (L07597), Phosphoglycerate mutase, muscle-specific (PGAM-M) (J05073), IP prostacyclin receptor (D38128), Pan-2 (HG2604-HT2700), Anion Exchanger 3 Cardiac Isom (HG4128-HT4398), Tax1 binding protein (U25801), Hepatic nuclear factor 1-alpha (TCF-1-alpha)/U73499 (U73499), M-phase phosphoprotein mpp9 (X98258), Brain 4 (X82324), PTX3/X97748; Also: M31166 (X97748), Uroporphyrinogen decarboxylase (URO-D)/M60891 (M60891), pTR7 repetitive sequence/X15675 (X15675), Erythropoietin receptor (M60459), Sulfite oxidase (L31573), HM145 (D10925), PEBP2aC1 acute myeloid leukaemia (Z35278), Trpc2 transcript (possible pseudo) (X89067), P3 (X12458), CD20 receptor (S7) (X07203), Aromatic amino acid decarboxylase (ddc) (M76180), DNA sequence from Huntington's Disease Region (Z69923), BAC clone GS244B22/7q21-q22/AC002450 (AC002450), Cysteine protease (D55696), Semaphorin (CD100) (U60800), DNA on chromosome 22q 11.2-qter contains GSTT1-2 (Z84718), WD repeat protein HAN11/U94747 (U94747), X64467_rna1 and others (M13928), Syt V (X96783), ltk; Also: D16105 (X52213), JTV-1 (JTV-1) (U24169), Alpha-L-iduronidase (M95740), Sterol carrier protein-X/sterol carrier protein-2 (SCP-X/SCP-2) (U11313), Aspartyl(asparaginyl)beta-hydroxylase; Also: U03109 (S83325), Presenilin 1 (PS1; S182); Also: L76517 (L76528), DAP-1 (X76105), SS-A/Ro ribonucleoprot autoantigen 60 kd subunit (M25077), Endothelin-B receptor (D13168), Ca2+-dependent activator protein secretion (U36448), Placenta (Diff33) (U49188), Putative OSP like protein (U89916), Peroxisomal 70 kD membrane protein; Also:X83467_rnal (M81182), Carnitine palmitoyltransferase II precursor (CPT1) (U09646), Isolate JuSo MUC18 glycoprot (3 variant); Also: M28882 (M29277), Cytochrome P450 (CYP2A13) (U22028), Cytochrome P450c21(M17252), and MBP1; Also: X15422 (X15954).
 48. The method of claims 20, or 21, wherein the at least one gene product further comprises: KIAA0006 (D13631), KIAA0010 (D13635), KIAA0053 (D29642), KIAA0060 (D31766), KIAA0064 (D31764), KIAA0066 (D31886), KIAA0079 (D38555), KIAA0086 (D42045), KIAA0091 (D42053), KIAA0092 (D42054), KIAA0100 (D43947), KIAA0133 (D50923), KIAA0150 KIAA0152 (D63486), (D63484), KIAA0187 (D80009), KIAA0201 (D86956), KIAA0217 (D86971), KLAA0230 (D86983), KIAA0235 (D87078), KIAA0240 (D87077), KIAA0260 (D87449), KIAA0281 (D87457), and KIAA0358 (AB002356).
 49. The method of claim 25, further comprising modulating the level of a gene product in Tables 16, 17 or 18, or CD18.
 50. A method of identifying a composition useful in the treatment or prevention of multiple sclerosis (MS) comprising: (a) providing a cell that expresses one or more genes identified in Tables 1-15, other than those indicated by an asterisk; (b) contacting said cell with a candidate substance; and (c) assessing the expression of the one or more genes, wherein modulation of the expression of the one or more genes identifies said candidate substances as a composition useful in the treatment or prevention of multiple sclerosis MS.
 51. The method of claim 48, wherein said cell is of neuronal, glial, endothelial, intravascular, perivascular, or central nervous system-infiltrating immune cell origin.
 52. The method of claim 49, wherein said neuronal cell is a neural progenitor or stem cell.
 53. The method of claim 49, wherein said glial cell is an astrocyte, microglia cell or oligodendrocyte.
 54. The method of claim 49, wherein said intravascular cell is a myocyte.
 55. The method of claim 49, wherein said perivascular cell is a pericyte.
 56. The method of claim 49, wherein said central nervous system-infiltrating immune cell is a lymphocyte, a monocyte, or a B cell. 